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Conserved domains on  [gi|1622892340|ref|XP_028694425|]
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unconventional myosin-If isoform X3 [Macaca mulatta]

Protein Classification

class I myosin( domain architecture ID 11544833)

class I myosin is an unconventional myosin that does not form dimers; it contains a a head/motor domain that has ATPase activity and functions as a molecular motor, utilizing ATP hydrolysis to generate directed movement toward the plus end along actin filaments

Graphical summary

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List of domain hits

Name Accession Description Interval E-value
MYSc_Myo1 cd01378
class I myosin, motor domain; Myosin I generates movement at the leading edge in cell motility, ...
31-677 0e+00

class I myosin, motor domain; Myosin I generates movement at the leading edge in cell motility, and class I myosins have been implicated in phagocytosis and vesicle transport. Myosin I, an unconventional myosin, does not form dimers. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. There are 5 myosin subclasses with subclasses c/h, d/g, and a/b have an IQ domain and a TH1 domain. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


:

Pssm-ID: 276829  Cd Length: 652  Bit Score: 1164.23  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   31 DAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISG 110
Cdd:cd01378      1 EAINENLKKRFENDEIYTYIGHVLISVNPFKDLGIYTDEVLESYRGKNRYEVPPHVFALADSAYRNMKSEKENQCVIISG 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  111 ESGAGKTVAAKYIMGYISKVSGGGN-KVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISN 189
Cdd:cd01378     81 ESGAGKTEASKRIMQYIAAVSGGSEsEVERVKDMLLASNPLLEAFGNAKTLRNDNSSRFGKYMEIQFDFKGEPVGGHITN 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  190 FLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSI 269
Cdd:cd01378    161 YLLEKSRVVGQIKGERNFHIFYQLLKGASQEYLQELGLQRPEQYYYYSKSGCFDVDGIDDAADFKEVLNAMKVIGFTEEE 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  270 QQLVLQLVAGILHLGNISFCEDGN-YARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSRWGGRSEsIDVTLNVEQAAY 348
Cdd:cd01378    241 QDSIFRILAAILHLGNIQFAEDEEgNAAISDTSVLDFVAYLLGVDPDQLEKALTHRTIETGGGGRSV-YEVPLNVEQAAY 319
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  349 TRDALAKGLYARLFDFLVEAINRAMQ--KPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEY 426
Cdd:cd01378    320 ARDALAKAIYSRLFDWIVERINKSLAakSGGKKKVIGVLDIYGFEIFEKNSFEQFCINYVNEKLQQIFIELTLKAEQEEY 399
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  427 VQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMhatGGGADQTLLQKLQAAVGTHEH-------FNSWSAG 499
Cdd:cd01378    400 VREGIEWTPIKYFNNKIICDLIEEK--PPGIFAILDDACLTA---GDATDQTFLQKLNQLFSNHPHfecpsghFELRRGE 474
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  500 FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKKGRPSTAGSKIKKQANDLVATLMRCTP 579
Cdd:cd01378    475 FRIKHYAGDVTYNVEGFLDKNKDLLFKDLKELMQSSSNPFLRSLFPEGVDLDSKKRPPTAGTKFKNSANALVETLMKKQP 554
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  580 HYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWRGDERQGVQHLLRA 659
Cdd:cd01378    555 SYIRCIKPNDNKSPGEFDEELVLHQVKYLGLLENVRVRRAGFAYRQTYEKFLERYKLLSPKTWPAWDGTWQGGVESILKD 634
                          650
                   ....*....|....*...
gi 1622892340  660 VNMEPDQYQMGSTKVFVK 677
Cdd:cd01378    635 LNIPPEEYQMGKTKIFIR 652
Myosin_TH1 pfam06017
Unconventional myosin tail, actin- and lipid-binding; Unconventional myosins, ie those that ...
750-946 2.13e-61

Unconventional myosin tail, actin- and lipid-binding; Unconventional myosins, ie those that are not found in muscle, have the common, classical-type head domain, sometimes a neck with the IQ calmodulin-binding motifs, and then non-standard tails. These tails determine the subcellular localization of the unconventional myosins and also help determine their individual functions. The family carries several different unconventional myosins, eg. Myo1f is expressed mainly in immune cells as well as in the inner ear where it can be associated with deafness, Myo1d has a lipid-binding module in their tail and is implicated in endosome vesicle recycling in epithelial cells. Myo1a, b, c and g from various eukaryotes are also found in this family.


:

Pssm-ID: 461801  Cd Length: 196  Bit Score: 207.84  E-value: 2.13e-61
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  750 AASNILLNKKERRRNSINRNFVGDYLGLEER-----PELRQFLGK--RERVDFADSVTKYDRRFKPIKRDLILTPKCVYV 822
Cdd:pfam06017    3 YASDLLKGRKERRRFSLLRRFMGDYLGLENNfsgpgPKLRKAVGIggDEKVLFSDRVSKFNRSSKPSPRILILTDKAVYL 82
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  823 IGREKVKKGpekgqVREVLKKKLDIQALRGVSLSTRQDDFFILQEDAV---DSFLESVFKTEFVSLLCKRFEEATRRPLP 899
Cdd:pfam06017   83 IDQKKLKNG-----LQYVLKRRIPLSDITGVSVSPLQDDWVVLHLGSPqkgDLLLECDFKTELVTHLSKAYKKKTNRKLN 157
                          170       180       190       200
                   ....*....|....*....|....*....|....*....|....*..
gi 1622892340  900 LTFSDTLQFRVKKegwggGGTRSVTFSRGSGDlavLKVGGRTLTVSV 946
Cdd:pfam06017  158 VKIGDTIEYRKKK-----GKIRTVKFVKDEPK---GKDSYKSGTVSV 196
SH3_MyoIe_If_like cd11827
Src homology 3 domain of Myosins Ie, If, and similar proteins; Myosins Ie (MyoIe) and If ...
1081-1133 1.71e-30

Src homology 3 domain of Myosins Ie, If, and similar proteins; Myosins Ie (MyoIe) and If (MyoIf) are nonmuscle, unconventional, long tailed, class I myosins containing an N-terminal motor domain and a myosin tail with TH1, TH2, and SH3 domains. MyoIe interacts with the endocytic proteins, dynamin and synaptojanin-1, through its SH3 domain; it may play a role in clathrin-dependent endocytosis. In the kidney, MyoIe is critical for podocyte function and normal glomerular filtration. Mutations in MyoIe is associated with focal segmental glomerulosclerosis, a disease characterized by massive proteinuria and progression to end-stage kidney disease. MyoIf is predominantly expressed in the immune system; it plays a role in immune cell motility and innate immunity. Mutations in MyoIf may be associated with the loss of hearing. The MyoIf gene has also been found to be fused to the MLL (Mixed lineage leukemia) gene in infant acute myeloid leukemias (AML). SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


:

Pssm-ID: 212761 [Multi-domain]  Cd Length: 53  Bit Score: 114.05  E-value: 1.71e-30
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11827      1 QCKALYAYDAQDTDELSFNEGDIIEILKEDPSGWWTGRLRGKEGLFPGNYVEK 53
PHA03378 super family cl33729
EBNA-3B; Provisional
947-1074 4.15e-08

EBNA-3B; Provisional


The actual alignment was detected with superfamily member PHA03378:

Pssm-ID: 223065 [Multi-domain]  Cd Length: 991  Bit Score: 57.77  E-value: 4.15e-08
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  947 GDGLPKSSKPTRK---GMAKGRPRRSSQAPTRAAPTRAAPGPPRGMDRNGVPPSA----RGGPLPLEimsggsshrPPRG 1019
Cdd:PHA03378   732 GRARPPAAAPGRArppAAAPGRARPPAAAPGRARPPAAAPGAPTPQPPPQAPPAPqqrpRGAPTPQP---------PPQA 802
                           90       100       110       120       130
                   ....*....|....*....|....*....|....*....|....*....|....*...
gi 1622892340 1020 PPSTSLGASRRPRAQL-PSEHNTEFLNVPD--QGMAGMqRKRSVGQRPVPGVGRPKPQ 1074
Cdd:PHA03378   803 GPTSMQLMPRAAPGQQgPTKQILRQLLTGGvkRGRPSL-KKPAALERQAAAGPTPSPG 859
 
Name Accession Description Interval E-value
MYSc_Myo1 cd01378
class I myosin, motor domain; Myosin I generates movement at the leading edge in cell motility, ...
31-677 0e+00

class I myosin, motor domain; Myosin I generates movement at the leading edge in cell motility, and class I myosins have been implicated in phagocytosis and vesicle transport. Myosin I, an unconventional myosin, does not form dimers. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. There are 5 myosin subclasses with subclasses c/h, d/g, and a/b have an IQ domain and a TH1 domain. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276829  Cd Length: 652  Bit Score: 1164.23  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   31 DAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISG 110
Cdd:cd01378      1 EAINENLKKRFENDEIYTYIGHVLISVNPFKDLGIYTDEVLESYRGKNRYEVPPHVFALADSAYRNMKSEKENQCVIISG 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  111 ESGAGKTVAAKYIMGYISKVSGGGN-KVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISN 189
Cdd:cd01378     81 ESGAGKTEASKRIMQYIAAVSGGSEsEVERVKDMLLASNPLLEAFGNAKTLRNDNSSRFGKYMEIQFDFKGEPVGGHITN 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  190 FLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSI 269
Cdd:cd01378    161 YLLEKSRVVGQIKGERNFHIFYQLLKGASQEYLQELGLQRPEQYYYYSKSGCFDVDGIDDAADFKEVLNAMKVIGFTEEE 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  270 QQLVLQLVAGILHLGNISFCEDGN-YARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSRWGGRSEsIDVTLNVEQAAY 348
Cdd:cd01378    241 QDSIFRILAAILHLGNIQFAEDEEgNAAISDTSVLDFVAYLLGVDPDQLEKALTHRTIETGGGGRSV-YEVPLNVEQAAY 319
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  349 TRDALAKGLYARLFDFLVEAINRAMQ--KPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEY 426
Cdd:cd01378    320 ARDALAKAIYSRLFDWIVERINKSLAakSGGKKKVIGVLDIYGFEIFEKNSFEQFCINYVNEKLQQIFIELTLKAEQEEY 399
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  427 VQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMhatGGGADQTLLQKLQAAVGTHEH-------FNSWSAG 499
Cdd:cd01378    400 VREGIEWTPIKYFNNKIICDLIEEK--PPGIFAILDDACLTA---GDATDQTFLQKLNQLFSNHPHfecpsghFELRRGE 474
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  500 FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKKGRPSTAGSKIKKQANDLVATLMRCTP 579
Cdd:cd01378    475 FRIKHYAGDVTYNVEGFLDKNKDLLFKDLKELMQSSSNPFLRSLFPEGVDLDSKKRPPTAGTKFKNSANALVETLMKKQP 554
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  580 HYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWRGDERQGVQHLLRA 659
Cdd:cd01378    555 SYIRCIKPNDNKSPGEFDEELVLHQVKYLGLLENVRVRRAGFAYRQTYEKFLERYKLLSPKTWPAWDGTWQGGVESILKD 634
                          650
                   ....*....|....*...
gi 1622892340  660 VNMEPDQYQMGSTKVFVK 677
Cdd:cd01378    635 LNIPPEEYQMGKTKIFIR 652
MYSc smart00242
Myosin. Large ATPases; ATPase; molecular motor. Muscle contraction consists of a cyclical ...
12-690 0e+00

Myosin. Large ATPases; ATPase; molecular motor. Muscle contraction consists of a cyclical interaction between myosin and actin. The core of the myosin structure is similar in fold to that of kinesin.


Pssm-ID: 214580 [Multi-domain]  Cd Length: 677  Bit Score: 1062.16  E-value: 0e+00
                            10        20        30        40        50        60        70        80
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340    12 HNVKQSGVDDMVLLPQITEDAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTD 91
Cdd:smart00242    1 NPPKFEGVEDLVLLTYLNEPAVLHNLKKRYLKDLIYTYIGLVLVAVNPYKQLPIYTDEVIKKYRGKSRGELPPHVFAIAD 80
                            90       100       110       120       130       140       150       160
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340    92 NMYRNMLIDCENQCVIISGESGAGKTVAAKYIMGYISKVSGGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKY 171
Cdd:smart00242   81 NAYRNMLNDKENQSIIISGESGAGKTENTKKIMQYLASVSGSNTEVGSVEDQILESNPILEAFGNAKTLRNNNSSRFGKF 160
                           170       180       190       200       210       220       230       240
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   172 FEIQFSRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRS 251
Cdd:smart00242  161 IEIHFDAKGKIIGAKIETYLLEKSRVVSQAKGERNYHIFYQLLAGASEELKKELGLKSPEDYRYLNQGGCLTVDGIDDAE 240
                           250       260       270       280       290       300       310       320
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   252 DFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISFCEDGNYAR---VESVDLLAFPAYLLGIDSGRLQEKLTSRKMDS 328
Cdd:smart00242  241 EFKETLNAMRVLGFSEEEQESIFKILAAILHLGNIEFEEGRNDNAastVKDKEELSNAAELLGVDPEELEKALTKRKIKT 320
                           330       340       350       360       370       380       390       400
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   329 RWggrsESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEE-YSIGVLDIYGFEIFQKNGFEQFCINFVN 407
Cdd:smart00242  321 GG----EVITKPLNVEQALDARDALAKALYSRLFDWLVKRINQSLSFKDGStYFIGVLDIYGFEIFEVNSFEQLCINYAN 396
                           410       420       430       440       450       460       470       480
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   408 EKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAV 487
Cdd:smart00242  397 EKLQQFFNQHVFKLEQEEYEREGIDWTFIDFFDNQDCIDLIEKK--PPGILSLLDEECRFPKGT----DQTFLEKLNQHH 470
                           490       500       510       520       530       540       550       560
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   488 GTHEHF----NSWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPE-KLDGDKKGRPSTAGSK 562
Cdd:smart00242  471 KKHPHFskpkKKGRTEFIIKHYAGDVTYDVTGFLEKNKDTLSDDLIELLQSSKNPLIASLFPSgVSNAGSKKRFQTVGSQ 550
                           570       580       590       600       610       620       630       640
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   563 IKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETW 642
Cdd:smart00242  551 FKEQLNELMDTLNSTNPHFIRCIKPNEEKKPGDFDSSLVLHQLRYLGVLENIRIRRAGFPYRLPFDEFLQRYRVLLPDTW 630
                           650       660       670       680
                    ....*....|....*....|....*....|....*....|....*...
gi 1622892340   643 PRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVKnPESLFLLEEVRE 690
Cdd:smart00242  631 PPWGGDAKKACEALLQSLGLDEDEYQLGKTKVFLR-PGQLAELEELRE 677
Myosin_head pfam00063
Myosin head (motor domain);
19-677 0e+00

Myosin head (motor domain);


Pssm-ID: 395017 [Multi-domain]  Cd Length: 674  Bit Score: 902.80  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   19 VDDMVLLPQITEDAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNML 98
Cdd:pfam00063    1 VEDMVELSYLNEPSVLHNLKKRYKSDLIYTYSGLVLVAVNPYKQLPIYSEDMIKAYRGKRRGELPPHIFAIADEAYRSML 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   99 IDCENQCVIISGESGAGKTVAAKYIMGYISKVSGGG--NKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQF 176
Cdd:pfam00063   81 QDKENQSILISGESGAGKTENTKKIMQYLASVSGSGsaGNVGRLEEQILQSNPILEAFGNAKTVRNNNSSRFGKYIEIQF 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  177 SRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGET 256
Cdd:pfam00063  161 DAKGDIVGGKIETYLLEKSRVVYQAEGERNYHIFYQLLAGASAQLKKELRLTNPKDYHYLSQSGCYTIDGIDDSEEFKIT 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  257 LSAMQVIGIPPSIQQLVLQLVAGILHLGNISFCED--GNYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRS 334
Cdd:pfam00063  241 DKAMDILGFSDEEQMGIFRIVAAILHLGNIEFKKErnDEQAVPDDTENLQKAASLLGIDSTELEKALCKRRIKT----GR 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  335 ESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS--IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQ 412
Cdd:pfam00063  317 ETVSKPQNVEQANYARDALAKAIYSRLFDWLVDRINKSLDVKTIEKAsfIGVLDIYGFEIFEKNSFEQLCINYVNEKLQQ 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  413 IFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEH 492
Cdd:pfam00063  397 FFNHHMFKLEQEEYVREGIEWTFIDFGDNQPCIDLIEKK--PLGILSLLDEECLFPKAT----DQTFLDKLYSTFSKHPH 470
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  493 FNSW----SAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP--EKLDGD-------------KK 553
Cdd:pfam00063  471 FQKPrlqgETHFIIKHYAGDVEYNVEGFLEKNKDPLNDDLVSLLKSSSDPLLAELFPdyETAESAaanesgkstpkrtKK 550
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  554 GRPSTAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQR 633
Cdd:pfam00063  551 KRFITVGSQFKESLGELMKTLNSTNPHYIRCIKPNEKKRAGVFDNSLVLHQLRCNGVLEGIRIRRAGFPNRITFQEFVQR 630
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|....
gi 1622892340  634 YAILTPETWPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:pfam00063  631 YRILAPKTWPKWKGDAKKGCEAILQSLNLDKEEYQFGKTKIFFR 674
COG5022 COG5022
Myosin heavy chain [General function prediction only];
12-886 0e+00

Myosin heavy chain [General function prediction only];


Pssm-ID: 227355 [Multi-domain]  Cd Length: 1463  Bit Score: 870.17  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   12 HNVKQSGVDDMVLLPQITEDAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTD 91
Cdd:COG5022     61 KLPKFDGVDDLTELSYLNEPAVLHNLEKRYNNGQIYTYSGLVLIAVNPYRDLGIYTDDIIQSYSGKNRLELEPHVFAIAE 140
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   92 NMYRNMLIDCENQCVIISGESGAGKTVAAKYIMGYISKVSGG-GNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGK 170
Cdd:COG5022    141 EAYRNLLSEKENQTIIISGESGAGKTENAKRIMQYLASVTSSsTVEISSIEKQILATNPILEAFGNAKTVRNDNSSRFGK 220
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  171 YFEIQFSRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDR 250
Cdd:COG5022    221 YIKIEFDENGEICGAKIETYLLEKSRVVHQNKNERNYHIFYQLLAGDPEELKKLLLLQNPKDYIYLSQGGCDKIDGIDDA 300
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  251 SDFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISFCEDGN-YARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSr 329
Cdd:COG5022    301 KEFKITLDALKTIGIDEEEQDQIFKILAAILHIGNIEFKEDRNgAAIFSDNSVLDKACYLLGIDPSLFVKWLVKRQIKT- 379
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  330 wggRSESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQE-EYSIGVLDIYGFEIFQKNGFEQFCINFVNE 408
Cdd:COG5022    380 ---GGEWIVVPLNLEQALAIRDSLAKALYSNLFDWIVDRINKSLDHSAAaSNFIGVLDIYGFEIFEKNSFEQLCINYTNE 456
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  409 KLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlSPPGIMSVLDDVCATMHATgggaDQTLLQKLQAA-- 486
Cdd:COG5022    457 KLQQFFNQHMFKLEQEEYVKEGIEWSFIDYFDNQPCIDLIEKK-NPLGILSLLDEECVMPHAT----DESFTSKLAQRln 531
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  487 VGTHEHFNSW---SAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKKGRPSTAGSKI 563
Cdd:COG5022    532 KNSNPKFKKSrfrDNKFVVKHYAGDVEYDVEGFLDKNKDPLNDDLLELLKASTNEFVSTLFDDEENIESKGRFPTLGSRF 611
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  564 KKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPE-TW 642
Cdd:COG5022    612 KESLNSLMSTLNSTQPHYIRCIKPNEEKSPWTFDNQMVLSQLRCCGVLETIRISRAGFPSRWTFDEFVQRYRILSPSkSW 691
                          650       660       670       680       690       700       710       720
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  643 P---RWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVKNPeSLFLLEEVRERKFDGFARTIQKAWRRHVAVRKYEEMREE 719
Cdd:COG5022    692 TgeyTWKEDTKNAVKSILEELVIDSSKYQIGNTKVFFKAG-VLAALEDMRDAKLDNIATRIQRAIRGRYLRRRYLQALKR 770
                          730       740       750       760       770       780       790       800
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  720 gERLWVHSAEWGRKdleepRQELCPPPSISAASNIllnkKERRRNSINRNFVGDYLGL--EERPELRQFLGKRERVDFAD 797
Cdd:COG5022    771 -IKKIQVIQHGFRL-----RRLVDYELKWRLFIKL----QPLLSLLGSRKEYRSYLACiiKLQKTIKREKKLRETEEVEF 840
                          810       820       830       840       850       860       870       880
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  798 S------VTKYDRRFKPIKRDLILTPKCVYVIGREKVKKGpekgqVREVLKKKLDIQALRGVSLSTRQDDFFIL---QED 868
Cdd:COG5022    841 SlkaevlIQKFGRSLKAKKRFSLLKKETIYLQSAQRVELA-----ERQLQELKIDVKSISSLKLVNLELESEIIelkKSL 915
                          890
                   ....*....|....*...
gi 1622892340  869 AVDSFLESVFKTEFVSLL 886
Cdd:COG5022    916 SSDLIENLEFKTELIARL 933
PTZ00014 PTZ00014
myosin-A; Provisional
19-715 1.40e-155

myosin-A; Provisional


Pssm-ID: 240229 [Multi-domain]  Cd Length: 821  Bit Score: 484.15  E-value: 1.40e-155
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   19 VDDMVLLPQITEDAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYEN-PPHIYALTDNMYRNM 97
Cdd:PTZ00014    98 YGDIGLLPHTNIPCVLDFLKHRYLKNQIYTTADPLLVAINPFKDLGNTTNDWIRRYRDAKDSDKlPPHVFTTARRALENL 177
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   98 LIDCENQCVIISGESGAGKTVAAKYIMGYISKvSGGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFS 177
Cdd:PTZ00014   178 HGVKKSQTIIVSGESGAGKTEATKQIMRYFAS-SKSGNMDLKIQNAIMAANPVLEAFGNAKTIRNNNSSRFGRFMQLQLG 256
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  178 RGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNqSDTYQVDGTDDRSDFGETL 257
Cdd:PTZ00014   257 EEGGIRYGSIVAFLLEKSRVVTQEDDERSYHIFYQLLKGANDEMKEKYKLKSLEEYKYIN-PKCLDVPGIDDVKDFEEVM 335
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  258 SAMQVIGIPPSIQQLVLQLVAGILHLGNISFCE-------DGNYARVESVDLLAFPAYLLGIDSGRLQEKLTsrkMDSRW 330
Cdd:PTZ00014   336 ESFDSMGLSESQIEDIFSILSGVLLLGNVEIEGkeeggltDAAAISDESLEVFNEACELLFLDYESLKKELT---VKVTY 412
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  331 GGRSEsIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQE-EYSIGVLDIYGFEIFQKNGFEQFCINFVNEK 409
Cdd:PTZ00014   413 AGNQK-IEGPWSKDESEMLKDSLSKAVYEKLFLWIIRNLNATIEPPGGfKVFIGMLDIFGFEVFKNNSLEQLFINITNEM 491
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  410 LQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKLSppGIMSVLDDVCATMhatgGGADQTLLQKLQAAVGT 489
Cdd:PTZ00014   492 LQKNFVDIVFERESKLYKDEGISTEELEYTSNESVIDLLCGKGK--SVLSILEDQCLAP----GGTDEKFVSSCNTNLKN 565
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  490 HEHF----NSWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP--EKLDGdKKGRPSTAGSKI 563
Cdd:PTZ00014   566 NPKYkpakVDSNKNFVIKHTIGDIQYCASGFLFKNKDVLRPELVEVVKASPNPLVRDLFEgvEVEKG-KLAKGQLIGSQF 644
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  564 KKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWP 643
Cdd:PTZ00014   645 LNQLDSLMSLINSTEPHFIRCIKPNENKKPLDWNSSKVLIQLHSLSILEALQLRQLGFSYRRTFAEFLSQFKYLDLAVSN 724
                          650       660       670       680       690       700       710
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....
gi 1622892340  644 RWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVKNPESLFLLEEVRER--KFDGFARTIQKAWRRHVAVRKYEE 715
Cdd:PTZ00014   725 DSSLDPKEKAEKLLERSGLPKDSYAIGKTMVFLKKDAAKELTQIQREKlaAWEPLVSVLEALILKIKKKRKVRK 798
Myosin_TH1 pfam06017
Unconventional myosin tail, actin- and lipid-binding; Unconventional myosins, ie those that ...
750-946 2.13e-61

Unconventional myosin tail, actin- and lipid-binding; Unconventional myosins, ie those that are not found in muscle, have the common, classical-type head domain, sometimes a neck with the IQ calmodulin-binding motifs, and then non-standard tails. These tails determine the subcellular localization of the unconventional myosins and also help determine their individual functions. The family carries several different unconventional myosins, eg. Myo1f is expressed mainly in immune cells as well as in the inner ear where it can be associated with deafness, Myo1d has a lipid-binding module in their tail and is implicated in endosome vesicle recycling in epithelial cells. Myo1a, b, c and g from various eukaryotes are also found in this family.


Pssm-ID: 461801  Cd Length: 196  Bit Score: 207.84  E-value: 2.13e-61
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  750 AASNILLNKKERRRNSINRNFVGDYLGLEER-----PELRQFLGK--RERVDFADSVTKYDRRFKPIKRDLILTPKCVYV 822
Cdd:pfam06017    3 YASDLLKGRKERRRFSLLRRFMGDYLGLENNfsgpgPKLRKAVGIggDEKVLFSDRVSKFNRSSKPSPRILILTDKAVYL 82
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  823 IGREKVKKGpekgqVREVLKKKLDIQALRGVSLSTRQDDFFILQEDAV---DSFLESVFKTEFVSLLCKRFEEATRRPLP 899
Cdd:pfam06017   83 IDQKKLKNG-----LQYVLKRRIPLSDITGVSVSPLQDDWVVLHLGSPqkgDLLLECDFKTELVTHLSKAYKKKTNRKLN 157
                          170       180       190       200
                   ....*....|....*....|....*....|....*....|....*..
gi 1622892340  900 LTFSDTLQFRVKKegwggGGTRSVTFSRGSGDlavLKVGGRTLTVSV 946
Cdd:pfam06017  158 VKIGDTIEYRKKK-----GKIRTVKFVKDEPK---GKDSYKSGTVSV 196
SH3_MyoIe_If_like cd11827
Src homology 3 domain of Myosins Ie, If, and similar proteins; Myosins Ie (MyoIe) and If ...
1081-1133 1.71e-30

Src homology 3 domain of Myosins Ie, If, and similar proteins; Myosins Ie (MyoIe) and If (MyoIf) are nonmuscle, unconventional, long tailed, class I myosins containing an N-terminal motor domain and a myosin tail with TH1, TH2, and SH3 domains. MyoIe interacts with the endocytic proteins, dynamin and synaptojanin-1, through its SH3 domain; it may play a role in clathrin-dependent endocytosis. In the kidney, MyoIe is critical for podocyte function and normal glomerular filtration. Mutations in MyoIe is associated with focal segmental glomerulosclerosis, a disease characterized by massive proteinuria and progression to end-stage kidney disease. MyoIf is predominantly expressed in the immune system; it plays a role in immune cell motility and innate immunity. Mutations in MyoIf may be associated with the loss of hearing. The MyoIf gene has also been found to be fused to the MLL (Mixed lineage leukemia) gene in infant acute myeloid leukemias (AML). SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212761 [Multi-domain]  Cd Length: 53  Bit Score: 114.05  E-value: 1.71e-30
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11827      1 QCKALYAYDAQDTDELSFNEGDIIEILKEDPSGWWTGRLRGKEGLFPGNYVEK 53
SH3 smart00326
Src homology 3 domains; Src homology 3 (SH3) domains bind to target proteins through sequences ...
1079-1132 3.78e-19

Src homology 3 domains; Src homology 3 (SH3) domains bind to target proteins through sequences containing proline and hydrophobic amino acids. Pro-containing polypeptides may bind to SH3 domains in 2 different binding orientations.


Pssm-ID: 214620 [Multi-domain]  Cd Length: 56  Bit Score: 81.82  E-value: 3.78e-19
                            10        20        30        40        50
                    ....*....|....*....|....*....|....*....|....*....|....*
gi 1622892340  1079 GPRCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLH-GQEGLFPGNYVE 1132
Cdd:smart00326    2 GPQVRALYDYTAQDPDELSFKKGDIITVLEKSDDGWWKGRLGrGKEGLFPSNYVE 56
SH3_9 pfam14604
Variant SH3 domain;
1084-1132 1.83e-13

Variant SH3 domain;


Pssm-ID: 434066 [Multi-domain]  Cd Length: 49  Bit Score: 65.72  E-value: 1.83e-13
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*....
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:pfam14604    1 ALYPYEPKDDDELSLQRGDVITVIEESEDGWWEGINTGRTGLVPANYVE 49
PHA03378 PHA03378
EBNA-3B; Provisional
947-1074 4.15e-08

EBNA-3B; Provisional


Pssm-ID: 223065 [Multi-domain]  Cd Length: 991  Bit Score: 57.77  E-value: 4.15e-08
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  947 GDGLPKSSKPTRK---GMAKGRPRRSSQAPTRAAPTRAAPGPPRGMDRNGVPPSA----RGGPLPLEimsggsshrPPRG 1019
Cdd:PHA03378   732 GRARPPAAAPGRArppAAAPGRARPPAAAPGRARPPAAAPGAPTPQPPPQAPPAPqqrpRGAPTPQP---------PPQA 802
                           90       100       110       120       130
                   ....*....|....*....|....*....|....*....|....*....|....*...
gi 1622892340 1020 PPSTSLGASRRPRAQL-PSEHNTEFLNVPD--QGMAGMqRKRSVGQRPVPGVGRPKPQ 1074
Cdd:PHA03378   803 GPTSMQLMPRAAPGQQgPTKQILRQLLTGGvkRGRPSL-KKPAALERQAAAGPTPSPG 859
Herpes_LP pfam03363
Herpesvirus leader protein;
952-1081 1.07e-03

Herpesvirus leader protein;


Pssm-ID: 281372 [Multi-domain]  Cd Length: 174  Bit Score: 41.24  E-value: 1.07e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  952 KSSKPTRKGMAKGRPRRSSQAPTRAAPTRAAPGPPRGmDRNGVPPSARGGPLPLEimsggsshrpPRGPPSTSLgasRRP 1031
Cdd:pfam03363   32 RSPSPTRGGQEPRRVRRRVLVQQEEEVVSGSPSGPRG-DRSEGPGPARPGPPGIG----------PEGPLGQLL---RRH 97
                           90       100       110       120       130
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1032 RAQLPSEHNTEFLNVPDQGMagMQRKRSVGQRPVPGVGRPKPQPRTHGPR 1081
Cdd:pfam03363   98 RSPSPTRGGQEPRRVRRRVL--VQQEEEVVSGSPSGPLRPRPQPPAQSLR 145
 
Name Accession Description Interval E-value
MYSc_Myo1 cd01378
class I myosin, motor domain; Myosin I generates movement at the leading edge in cell motility, ...
31-677 0e+00

class I myosin, motor domain; Myosin I generates movement at the leading edge in cell motility, and class I myosins have been implicated in phagocytosis and vesicle transport. Myosin I, an unconventional myosin, does not form dimers. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. There are 5 myosin subclasses with subclasses c/h, d/g, and a/b have an IQ domain and a TH1 domain. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276829  Cd Length: 652  Bit Score: 1164.23  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   31 DAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISG 110
Cdd:cd01378      1 EAINENLKKRFENDEIYTYIGHVLISVNPFKDLGIYTDEVLESYRGKNRYEVPPHVFALADSAYRNMKSEKENQCVIISG 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  111 ESGAGKTVAAKYIMGYISKVSGGGN-KVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISN 189
Cdd:cd01378     81 ESGAGKTEASKRIMQYIAAVSGGSEsEVERVKDMLLASNPLLEAFGNAKTLRNDNSSRFGKYMEIQFDFKGEPVGGHITN 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  190 FLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSI 269
Cdd:cd01378    161 YLLEKSRVVGQIKGERNFHIFYQLLKGASQEYLQELGLQRPEQYYYYSKSGCFDVDGIDDAADFKEVLNAMKVIGFTEEE 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  270 QQLVLQLVAGILHLGNISFCEDGN-YARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSRWGGRSEsIDVTLNVEQAAY 348
Cdd:cd01378    241 QDSIFRILAAILHLGNIQFAEDEEgNAAISDTSVLDFVAYLLGVDPDQLEKALTHRTIETGGGGRSV-YEVPLNVEQAAY 319
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  349 TRDALAKGLYARLFDFLVEAINRAMQ--KPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEY 426
Cdd:cd01378    320 ARDALAKAIYSRLFDWIVERINKSLAakSGGKKKVIGVLDIYGFEIFEKNSFEQFCINYVNEKLQQIFIELTLKAEQEEY 399
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  427 VQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMhatGGGADQTLLQKLQAAVGTHEH-------FNSWSAG 499
Cdd:cd01378    400 VREGIEWTPIKYFNNKIICDLIEEK--PPGIFAILDDACLTA---GDATDQTFLQKLNQLFSNHPHfecpsghFELRRGE 474
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  500 FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKKGRPSTAGSKIKKQANDLVATLMRCTP 579
Cdd:cd01378    475 FRIKHYAGDVTYNVEGFLDKNKDLLFKDLKELMQSSSNPFLRSLFPEGVDLDSKKRPPTAGTKFKNSANALVETLMKKQP 554
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  580 HYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWRGDERQGVQHLLRA 659
Cdd:cd01378    555 SYIRCIKPNDNKSPGEFDEELVLHQVKYLGLLENVRVRRAGFAYRQTYEKFLERYKLLSPKTWPAWDGTWQGGVESILKD 634
                          650
                   ....*....|....*...
gi 1622892340  660 VNMEPDQYQMGSTKVFVK 677
Cdd:cd01378    635 LNIPPEEYQMGKTKIFIR 652
MYSc smart00242
Myosin. Large ATPases; ATPase; molecular motor. Muscle contraction consists of a cyclical ...
12-690 0e+00

Myosin. Large ATPases; ATPase; molecular motor. Muscle contraction consists of a cyclical interaction between myosin and actin. The core of the myosin structure is similar in fold to that of kinesin.


Pssm-ID: 214580 [Multi-domain]  Cd Length: 677  Bit Score: 1062.16  E-value: 0e+00
                            10        20        30        40        50        60        70        80
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340    12 HNVKQSGVDDMVLLPQITEDAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTD 91
Cdd:smart00242    1 NPPKFEGVEDLVLLTYLNEPAVLHNLKKRYLKDLIYTYIGLVLVAVNPYKQLPIYTDEVIKKYRGKSRGELPPHVFAIAD 80
                            90       100       110       120       130       140       150       160
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340    92 NMYRNMLIDCENQCVIISGESGAGKTVAAKYIMGYISKVSGGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKY 171
Cdd:smart00242   81 NAYRNMLNDKENQSIIISGESGAGKTENTKKIMQYLASVSGSNTEVGSVEDQILESNPILEAFGNAKTLRNNNSSRFGKF 160
                           170       180       190       200       210       220       230       240
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   172 FEIQFSRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRS 251
Cdd:smart00242  161 IEIHFDAKGKIIGAKIETYLLEKSRVVSQAKGERNYHIFYQLLAGASEELKKELGLKSPEDYRYLNQGGCLTVDGIDDAE 240
                           250       260       270       280       290       300       310       320
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   252 DFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISFCEDGNYAR---VESVDLLAFPAYLLGIDSGRLQEKLTSRKMDS 328
Cdd:smart00242  241 EFKETLNAMRVLGFSEEEQESIFKILAAILHLGNIEFEEGRNDNAastVKDKEELSNAAELLGVDPEELEKALTKRKIKT 320
                           330       340       350       360       370       380       390       400
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   329 RWggrsESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEE-YSIGVLDIYGFEIFQKNGFEQFCINFVN 407
Cdd:smart00242  321 GG----EVITKPLNVEQALDARDALAKALYSRLFDWLVKRINQSLSFKDGStYFIGVLDIYGFEIFEVNSFEQLCINYAN 396
                           410       420       430       440       450       460       470       480
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   408 EKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAV 487
Cdd:smart00242  397 EKLQQFFNQHVFKLEQEEYEREGIDWTFIDFFDNQDCIDLIEKK--PPGILSLLDEECRFPKGT----DQTFLEKLNQHH 470
                           490       500       510       520       530       540       550       560
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   488 GTHEHF----NSWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPE-KLDGDKKGRPSTAGSK 562
Cdd:smart00242  471 KKHPHFskpkKKGRTEFIIKHYAGDVTYDVTGFLEKNKDTLSDDLIELLQSSKNPLIASLFPSgVSNAGSKKRFQTVGSQ 550
                           570       580       590       600       610       620       630       640
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   563 IKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETW 642
Cdd:smart00242  551 FKEQLNELMDTLNSTNPHFIRCIKPNEEKKPGDFDSSLVLHQLRYLGVLENIRIRRAGFPYRLPFDEFLQRYRVLLPDTW 630
                           650       660       670       680
                    ....*....|....*....|....*....|....*....|....*...
gi 1622892340   643 PRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVKnPESLFLLEEVRE 690
Cdd:smart00242  631 PPWGGDAKKACEALLQSLGLDEDEYQLGKTKVFLR-PGQLAELEELRE 677
Myosin_head pfam00063
Myosin head (motor domain);
19-677 0e+00

Myosin head (motor domain);


Pssm-ID: 395017 [Multi-domain]  Cd Length: 674  Bit Score: 902.80  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   19 VDDMVLLPQITEDAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNML 98
Cdd:pfam00063    1 VEDMVELSYLNEPSVLHNLKKRYKSDLIYTYSGLVLVAVNPYKQLPIYSEDMIKAYRGKRRGELPPHIFAIADEAYRSML 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   99 IDCENQCVIISGESGAGKTVAAKYIMGYISKVSGGG--NKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQF 176
Cdd:pfam00063   81 QDKENQSILISGESGAGKTENTKKIMQYLASVSGSGsaGNVGRLEEQILQSNPILEAFGNAKTVRNNNSSRFGKYIEIQF 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  177 SRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGET 256
Cdd:pfam00063  161 DAKGDIVGGKIETYLLEKSRVVYQAEGERNYHIFYQLLAGASAQLKKELRLTNPKDYHYLSQSGCYTIDGIDDSEEFKIT 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  257 LSAMQVIGIPPSIQQLVLQLVAGILHLGNISFCED--GNYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRS 334
Cdd:pfam00063  241 DKAMDILGFSDEEQMGIFRIVAAILHLGNIEFKKErnDEQAVPDDTENLQKAASLLGIDSTELEKALCKRRIKT----GR 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  335 ESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS--IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQ 412
Cdd:pfam00063  317 ETVSKPQNVEQANYARDALAKAIYSRLFDWLVDRINKSLDVKTIEKAsfIGVLDIYGFEIFEKNSFEQLCINYVNEKLQQ 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  413 IFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEH 492
Cdd:pfam00063  397 FFNHHMFKLEQEEYVREGIEWTFIDFGDNQPCIDLIEKK--PLGILSLLDEECLFPKAT----DQTFLDKLYSTFSKHPH 470
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  493 FNSW----SAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP--EKLDGD-------------KK 553
Cdd:pfam00063  471 FQKPrlqgETHFIIKHYAGDVEYNVEGFLEKNKDPLNDDLVSLLKSSSDPLLAELFPdyETAESAaanesgkstpkrtKK 550
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  554 GRPSTAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQR 633
Cdd:pfam00063  551 KRFITVGSQFKESLGELMKTLNSTNPHYIRCIKPNEKKRAGVFDNSLVLHQLRCNGVLEGIRIRRAGFPNRITFQEFVQR 630
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|....
gi 1622892340  634 YAILTPETWPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:pfam00063  631 YRILAPKTWPKWKGDAKKGCEAILQSLNLDKEEYQFGKTKIFFR 674
COG5022 COG5022
Myosin heavy chain [General function prediction only];
12-886 0e+00

Myosin heavy chain [General function prediction only];


Pssm-ID: 227355 [Multi-domain]  Cd Length: 1463  Bit Score: 870.17  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   12 HNVKQSGVDDMVLLPQITEDAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTD 91
Cdd:COG5022     61 KLPKFDGVDDLTELSYLNEPAVLHNLEKRYNNGQIYTYSGLVLIAVNPYRDLGIYTDDIIQSYSGKNRLELEPHVFAIAE 140
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   92 NMYRNMLIDCENQCVIISGESGAGKTVAAKYIMGYISKVSGG-GNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGK 170
Cdd:COG5022    141 EAYRNLLSEKENQTIIISGESGAGKTENAKRIMQYLASVTSSsTVEISSIEKQILATNPILEAFGNAKTVRNDNSSRFGK 220
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  171 YFEIQFSRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDR 250
Cdd:COG5022    221 YIKIEFDENGEICGAKIETYLLEKSRVVHQNKNERNYHIFYQLLAGDPEELKKLLLLQNPKDYIYLSQGGCDKIDGIDDA 300
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  251 SDFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISFCEDGN-YARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSr 329
Cdd:COG5022    301 KEFKITLDALKTIGIDEEEQDQIFKILAAILHIGNIEFKEDRNgAAIFSDNSVLDKACYLLGIDPSLFVKWLVKRQIKT- 379
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  330 wggRSESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQE-EYSIGVLDIYGFEIFQKNGFEQFCINFVNE 408
Cdd:COG5022    380 ---GGEWIVVPLNLEQALAIRDSLAKALYSNLFDWIVDRINKSLDHSAAaSNFIGVLDIYGFEIFEKNSFEQLCINYTNE 456
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  409 KLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlSPPGIMSVLDDVCATMHATgggaDQTLLQKLQAA-- 486
Cdd:COG5022    457 KLQQFFNQHMFKLEQEEYVKEGIEWSFIDYFDNQPCIDLIEKK-NPLGILSLLDEECVMPHAT----DESFTSKLAQRln 531
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  487 VGTHEHFNSW---SAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKKGRPSTAGSKI 563
Cdd:COG5022    532 KNSNPKFKKSrfrDNKFVVKHYAGDVEYDVEGFLDKNKDPLNDDLLELLKASTNEFVSTLFDDEENIESKGRFPTLGSRF 611
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  564 KKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPE-TW 642
Cdd:COG5022    612 KESLNSLMSTLNSTQPHYIRCIKPNEEKSPWTFDNQMVLSQLRCCGVLETIRISRAGFPSRWTFDEFVQRYRILSPSkSW 691
                          650       660       670       680       690       700       710       720
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  643 P---RWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVKNPeSLFLLEEVRERKFDGFARTIQKAWRRHVAVRKYEEMREE 719
Cdd:COG5022    692 TgeyTWKEDTKNAVKSILEELVIDSSKYQIGNTKVFFKAG-VLAALEDMRDAKLDNIATRIQRAIRGRYLRRRYLQALKR 770
                          730       740       750       760       770       780       790       800
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  720 gERLWVHSAEWGRKdleepRQELCPPPSISAASNIllnkKERRRNSINRNFVGDYLGL--EERPELRQFLGKRERVDFAD 797
Cdd:COG5022    771 -IKKIQVIQHGFRL-----RRLVDYELKWRLFIKL----QPLLSLLGSRKEYRSYLACiiKLQKTIKREKKLRETEEVEF 840
                          810       820       830       840       850       860       870       880
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  798 S------VTKYDRRFKPIKRDLILTPKCVYVIGREKVKKGpekgqVREVLKKKLDIQALRGVSLSTRQDDFFIL---QED 868
Cdd:COG5022    841 SlkaevlIQKFGRSLKAKKRFSLLKKETIYLQSAQRVELA-----ERQLQELKIDVKSISSLKLVNLELESEIIelkKSL 915
                          890
                   ....*....|....*...
gi 1622892340  869 AVDSFLESVFKTEFVSLL 886
Cdd:COG5022    916 SSDLIENLEFKTELIARL 933
MYSc cd00124
Myosin motor domain superfamily; Myosin motor domain. The catalytic (head) domain has ATPase ...
31-677 0e+00

Myosin motor domain superfamily; Myosin motor domain. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276950 [Multi-domain]  Cd Length: 633  Bit Score: 765.21  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   31 DAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAA-QYENPPHIYALTDNMYRNMLIDCENQCVIIS 109
Cdd:cd00124      1 AAILHNLRERYARDLIYTYVGDILVAVNPFKWLPLYSEEVMEKYRGKGrSADLPPHVFAVADAAYRAMLRDGQNQSILIS 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  110 GESGAGKTVAAKYIMGYISKVSGGGNKVQHVK-----DIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDG 184
Cdd:cd00124     81 GESGAGKTETTKLVLKYLAALSGSGSSKSSSSassieQQILQSNPILEAFGNAKTVRNDNSSRFGKFIELQFDPTGRLVG 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  185 GKISNFLLEKSRVVMQNENERNFHIYYQLL----EGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAM 260
Cdd:cd00124    161 ASIETYLLEKSRVVSQAPGERNFHIFYQLLaglsDGAREELKLELLLSYYYLNDYLNSSGCDRIDGVDDAEEFQELLDAL 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  261 QVIGIPPSIQQLVLQLVAGILHLGNISFCEDGN----YARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSES 336
Cdd:cd00124    241 DVLGFSDEEQDSIFRILAAILHLGNIEFEEDEEdedsSAEVADDESLKAAAKLLGVDAEDLEEALTTRTIKV----GGET 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  337 IDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQ---KPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQI 413
Cdd:cd00124    317 ITKPLTVEQAEDARDALAKALYSRLFDWLVNRINAALSptdAAESTSFIGILDIFGFENFEVNSFEQLCINYANEKLQQF 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  414 FIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHF 493
Cdd:cd00124    397 FNQHVFKLEQEEYEEEGIDWSFIDFPDNQDCLDLIEGK--PLGILSLLDEECLFPKGT----DATFLEKLYSAHGSHPRF 470
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  494 NS----WSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTseqaflrmlfpekldgdkkgrpstaGSKIKKQAND 569
Cdd:cd00124    471 FSkkrkAKLEFGIKHYAGDVTYDADGFLEKNKDTLPPDLVDLLRS-------------------------GSQFRSQLDA 525
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  570 LVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWRGDE 649
Cdd:cd00124    526 LMDTLNSTQPHFVRCIKPNDEKKPGLFDPELVLEQLRCAGVLEAVRIRRAGYPVRLPFDEFLKRYRILAPGATEKASDSK 605
                          650       660
                   ....*....|....*....|....*...
gi 1622892340  650 RQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd00124    606 KAAVLALLLLLKLDSSGYQLGKTKVFLR 633
MYSc_Myo5 cd01380
class V myosin, motor domain; Myo5, also called heavy chain 12, myoxin, are dimeric myosins ...
36-675 0e+00

class V myosin, motor domain; Myo5, also called heavy chain 12, myoxin, are dimeric myosins that transport a variety of intracellular cargo processively along actin filaments, such as melanosomes, synaptic vesicles, vacuoles, and mRNA. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. It also contains a IQ domain and a globular DIL domain. Myosin V is a class of actin-based motor proteins involved in cytoplasmic vesicle transport and anchorage, spindle-pole alignment and mRNA translocation. The protein encoded by this gene is abundant in melanocytes and nerve cells. Mutations in this gene cause Griscelli syndrome type-1 (GS1), Griscelli syndrome type-3 (GS3) and neuroectodermal melanolysosomal disease, or Elejalde disease. Multiple alternatively spliced transcript variants encoding different isoforms have been reported, but the full-length nature of some variants has not been determined. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. Note that the Dictyostelium myoVs are not contained in this child group. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276831 [Multi-domain]  Cd Length: 629  Bit Score: 664.62  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMD-DYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGA 114
Cdd:cd01380      6 NLKVRFCQrNAIYTYCGIVLVAINPYEDLPIYGEDIIQAYSGQNMGELDPHIFAIAEEAYRQMARDEKNQSIIVSGESGA 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  115 GKTVAAKYIMGYISKVSGGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNFLLEK 194
Cdd:cd01380     86 GKTVSAKYAMRYFATVGGSSSGETQVEEKVLASNPIMEAFGNAKTTRNDNSSRFGKYIEILFDKNYRIIGANMRTYLLEK 165
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  195 SRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSIQQLVL 274
Cdd:cd01380    166 SRVVFQAEEERNYHIFYQLCAAASLPELKELHLGSAEDFFYTNQGGSPVIDGVDDAAEFEETRKALTLLGISEEEQMEIF 245
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  275 QLVAGILHLGNISFCEDGNY-ARVESVDL-LAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNVEQAAYTRDA 352
Cdd:cd01380    246 RILAAILHLGNVEIKATRNDsASISPDDEhLQIACELLGIDESQLAKWLCKRKIVT----RSEVIVKPLTLQQAIVARDA 321
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  353 LAKGLYARLFDFLVEAINRAM---QKPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQE 429
Cdd:cd01380    322 LAKHIYAQLFDWIVDRINKALaspVKEKQHSFIGVLDIYGFETFEVNSFEQFCINYANEKLQQQFNQHVFKLEQEEYVKE 401
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  430 GIRWTPIQYFNNKVVCDLIENKLsppGIMSVLDDVCaTMhatGGGADQTLLQKL--QAAVGTHEHFNS--WSAG-FVIHH 504
Cdd:cd01380    402 EIEWSFIDFYDNQPCIDLIEGKL---GILDLLDEEC-RL---PKGSDENWAQKLynQHLKKPNKHFKKprFSNTaFIVKH 474
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  505 YAGKVSYDVSGFCERNRDVLFSDLIELMQTSeqaflrmlfpekldgdkKGRPSTAGSKIKKQANDLVATLMRCTPHYIRC 584
Cdd:cd01380    475 FADDVEYQVEGFLEKNRDTVSEEHLNVLKAS-----------------KNRKKTVGSQFRDSLILLMETLNSTTPHYVRC 537
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  585 IKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETwPRWRGDERQGVQHLLRAVNMEP 664
Cdd:cd01380    538 IKPNDEKLPFTFDPKRVVQQLRACGVLETIRISAAGFPSRWTYEEFFSRYRVLLPSK-EWLRDDKKKTCENILENLILDP 616
                          650
                   ....*....|.
gi 1622892340  665 DQYQMGSTKVF 675
Cdd:cd01380    617 DKYQFGKTKIF 627
MYSc_Myo7 cd01381
class VII myosin, motor domain; These monomeric myosins have been associated with functions in ...
32-677 0e+00

class VII myosin, motor domain; These monomeric myosins have been associated with functions in sensory systems such as vision and hearing. Mammalian myosin VII has a tail with 2 MyTH4 domains, 2 FERM domains, and a SH3 domain. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276832  Cd Length: 648  Bit Score: 662.80  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd01381      2 GILRNLLIRYREKLIYTYTGSILVAVNPYQILPIYTAEQIRLYRNKKIGELPPHIFAIADNAYTNMKRNKRDQCVVISGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGggnkvQH--VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISN 189
Cdd:cd01381     82 SGAGKTESTKLILQYLAAISG-----QHswIEQQILEANPILEAFGNAKTIRNDNSSRFGKYIDIHFNKNGVIEGAKIEQ 156
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  190 FLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSI 269
Cdd:cd01381    157 YLLEKSRIVSQAPDERNYHIFYCMLAGLSAEEKKKLELGDASDYYYLTQGNCLTCEGRDDAAEFADIRSAMKVLMFTDEE 236
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  270 QQLVLQLVAGILHLGNISFcEDGNYARVESVDL-----LAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNVE 344
Cdd:cd01381    237 IWDIFKLLAAILHLGNIKF-EATVVDNLDASEVrdppnLERAAKLLEVPKQDLVDALTTRTIFT----RGETVVSPLSAE 311
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  345 QAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEE----YSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLK 420
Cdd:cd01381    312 QALDVRDAFVKGIYGRLFIWIVNKINSAIYKPRGTdssrTSIGVLDIFGFENFEVNSFEQLCINFANENLQQFFVRHIFK 391
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  421 AEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHF----NSW 496
Cdd:cd01381    392 LEQEEYDKEGINWQHIEFVDNQDVLDLIALK--PMNIMSLIDEESKFPKGT----DQTMLEKLHSTHGNNKNYlkpkSDL 465
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  497 SAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKL--DGDKKGRPSTAGSKIKKQANDLVATL 574
Cdd:cd01381    466 NTSFGINHFAGVVFYDTRGFLEKNRDTFSADLLQLVQSSKNKFLKQLFNEDIsmGSETRKKSPTLSSQFRKSLDQLMKTL 545
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  575 MRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWRGDERQGVQ 654
Cdd:cd01381    546 SACQPFFVRCIKPNEYKKPMLFDRELCVRQLRYSGMMETIRIRKAGYPIRHTFEEFVERYRVLVPGIPPAHKTDCRAATR 625
                          650       660
                   ....*....|....*....|...
gi 1622892340  655 HLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd01381    626 KICCAVLGGDADYQLGKTKIFLK 648
MYSc_class_II cd01377
class II myosins, motor domain; Myosin motor domain in class II myosins. Class II myosins, ...
36-677 0e+00

class II myosins, motor domain; Myosin motor domain in class II myosins. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. Thus, myosin II has two heads. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276951 [Multi-domain]  Cd Length: 662  Bit Score: 661.47  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGAG 115
Cdd:cd01377      6 NLRERYYSDLIYTYSGLFCVAVNPYKRLPIYTEEVIDKYKGKRREEMPPHIFAIADNAYRNMLQDRENQSILITGESGAG 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  116 KTVAAKYIMGYISKVSGGGNKVQHVKDI-------ILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKIS 188
Cdd:cd01377     86 KTENTKKVIQYLASVAASSKKKKESGKKkgtledqILQANPILEAFGNAKTVRNNNSSRFGKFIRIHFGSTGKIAGADIE 165
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  189 NFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPS 268
Cdd:cd01377    166 TYLLEKSRVVRQAKGERNYHIFYQLLSGADPELKEKLLLTGDPSYYFFLSQGELTIDGVDDAEEFKLTDEAFDILGFSEE 245
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  269 IQQLVLQLVAGILHLGNISFCEDGN--YARVESVDLLAFPAYLLGIDSGRLQEKLTSRKmdSRWGgrSESIDVTLNVEQA 346
Cdd:cd01377    246 EKMSIFKIVAAILHLGNIKFKQRRReeQAELDGTEEADKAAHLLGVNSSDLLKALLKPR--IKVG--REWVTKGQNKEQV 321
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  347 AYTRDALAKGLYARLFDFLVEAINRAMQKPQE-EYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIF----IELtlka 421
Cdd:cd01377    322 VFSVGALAKALYERLFLWLVKRINKTLDTKSKrQYFIGVLDIAGFEIFEFNSFEQLCINYTNEKLQQFFnhhmFVL---- 397
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  422 EQEEYVQEGIRWTPIQYFNNKVVC-DLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNSWS--- 497
Cdd:cd01377    398 EQEEYKKEGIEWTFIDFGLDLQPTiDLIEKP--NMGILSILDEECVFPKAT----DKTFVEKLYSNHLGKSKNFKKPkpk 471
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  498 ---AGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGD--------KKGRPSTAGSKIKKQ 566
Cdd:cd01377    472 kseAHFILKHYAGDVEYNIDGWLEKNKDPLNENVVALLKKSSDPLVASLFKDYEESGggggkkkkKGGSFRTVSQLHKEQ 551
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  567 ANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWR 646
Cdd:cd01377    552 LNKLMTTLRSTHPHFVRCIIPNEEKKPGKIDAPLVLHQLRCNGVLEGIRICRKGFPNRIIFAEFKQRYSILAPNAIPKGF 631
                          650       660       670
                   ....*....|....*....|....*....|.
gi 1622892340  647 GDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd01377    632 DDGKAACEKILKALQLDPELYRIGNTKVFFK 662
MYSc_Myo11 cd01384
class XI myosin, motor domain; These plant-specific type XI myosin are involved in organelle ...
36-677 0e+00

class XI myosin, motor domain; These plant-specific type XI myosin are involved in organelle transport. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle.


Pssm-ID: 276835  Cd Length: 647  Bit Score: 660.52  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREI-DLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGA 114
Cdd:cd01384      6 NLKVRYELDEIYTYTGNILIAVNPFKRLPHLYDAHMmEQYKGAPLGELSPHVFAVADAAYRAMINEGKSQSILVSGESGA 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  115 GKTVAAKYIMGYISKVSGGGN-KVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNFLLE 193
Cdd:cd01384     86 GKTETTKMLMQYLAYMGGRAVtEGRSVEQQVLESNPLLEAFGNAKTVRNNNSSRFGKFVEIQFDDAGRISGAAIRTYLLE 165
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  194 KSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSIQQLV 273
Cdd:cd01384    166 RSRVVQVSDPERNYHCFYQLCAGAPPEDREKYKLKDPKQFHYLNQSKCFELDGVDDAEEYRATRRAMDVVGISEEEQDAI 245
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  274 LQLVAGILHLGNISFC---EDGNYARV--ESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNVEQAAY 348
Cdd:cd01384    246 FRVVAAILHLGNIEFSkgeEDDSSVPKdeKSEFHLKAAAELLMCDEKALEDALCKRVIVT----PDGIITKPLDPDAATL 321
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  349 TRDALAKGLYARLFDFLVEAINRAM-QKPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYV 427
Cdd:cd01384    322 SRDALAKTIYSRLFDWLVDKINRSIgQDPNSKRLIGVLDIYGFESFKTNSFEQFCINLANEKLQQHFNQHVFKMEQEEYT 401
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  428 QEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFN----SWSAgFVIH 503
Cdd:cd01384    402 KEEIDWSYIEFVDNQDVLDLIEKK--PGGIIALLDEACMFPRST----HETFAQKLYQTLKDHKRFSkpklSRTD-FTID 474
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  504 HYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGD--KKGRPSTAGSKIKKQANDLVATLMRCTPHY 581
Cdd:cd01384    475 HYAGDVTYQTDLFLDKNKDYVVAEHQALLNASKCPFVAGLFPPLPREGtsSSSKFSSIGSRFKQQLQELMETLNTTEPHY 554
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  582 IRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETwPRWRGDERQGVQHLLRAVN 661
Cdd:cd01384    555 IRCIKPNNLLKPGIFENANVLQQLRCGGVLEAVRISCAGYPTRKPFEEFLDRFGLLAPEV-LKGSDDEKAACKKILEKAG 633
                          650
                   ....*....|....*.
gi 1622892340  662 MEpdQYQMGSTKVFVK 677
Cdd:cd01384    634 LK--GYQIGKTKVFLR 647
MYSc_Myo22 cd14883
class XXII myosin, motor domain; These myosins possess an extended neck with multiple IQ ...
32-677 0e+00

class XXII myosin, motor domain; These myosins possess an extended neck with multiple IQ motifs such as found in class V, VIII, XI, and XIII myosins. These myosins are defined by two tandem MyTH4 and FERM domains. The apicomplexan, but not diatom myosins contain 4-6 WD40 repeats near the end of the C-terminal tail which suggests a possible function of these myosins in signal transduction and transcriptional regulation. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276849 [Multi-domain]  Cd Length: 661  Bit Score: 660.17  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14883      2 GINTNLKVRYKKDLIYTYTGSILVAVNPYKELPIYTQDIVKQYFGKRMGALPPHIFALAEAAYTNMQEDGKNQSVIISGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVsggGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNFL 191
Cdd:cd14883     82 SGAGKTETTKLILQYLCAV---TNNHSWVEQQILEANTILEAFGNAKTVRNDNSSRFGKFIEVCFDASGHIKGAIIQDYL 158
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  192 LEKSRVVMQNENERNFHIYYQLLEGA--SQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSI 269
Cdd:cd14883    159 LEQSRITFQAPGERNYHVFYQLLAGAkhSKELKEKLKLGEPEDYHYLNQSGCIRIDNINDKKDFDHLRLAMNVLGIPEEM 238
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  270 QQLVLQLVAGILHLGNISFCE-DGNYA--RVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNVEQA 346
Cdd:cd14883    239 QEGIFSVLSAILHLGNLTFEDiDGETGalTVEDKEILKIVAKLLGVDPDKLKKALTIRQINV----RGNVTEIPLKVQEA 314
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  347 AYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS-IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEE 425
Cdd:cd14883    315 RDNRDAMAKALYSRTFAWLVNHINSCTNPGQKNSRfIGVLDIFGFENFKVNSFEQLCINYTNEKLHKFFNHYVFKLEQEE 394
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  426 YVQEGIRWTPIQYFNNKVVCDLIENklSPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHF-----NSWSAGF 500
Cdd:cd14883    395 YEKEGINWSHIVFTDNQECLDLIEK--PPLGILKLLDEECRFPKGT----DLTYLEKLHAAHEKHPYYekpdrRRWKTEF 468
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  501 VIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLF-PEKLD----------------GDKKGRPsTAGSKI 563
Cdd:cd14883    469 GVKHYAGEVTYTVQGFLDKNKDTQQDDLFDLMSRSKNKFVKELFtYPDLLaltglsislggdttsrGTSKGKP-TVGDTF 547
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  564 KKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWP 643
Cdd:cd14883    548 KHQLQSLVDVLSATQPWYVRCIKPNSLKEPNVFDDELVLAQLRYAGMLEIIRIRKEGFPIHLTFKEFVDRYLCLDPRARS 627
                          650       660       670
                   ....*....|....*....|....*....|....
gi 1622892340  644 RWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14883    628 ADHKETCGAVRALMGLGGLPEDEWQVGKTKVFLR 661
MYSc_Myo8 cd01383
class VIII myosin, motor domain; These plant-specific type VIII myosins has been associated ...
32-677 0e+00

class VIII myosin, motor domain; These plant-specific type VIII myosins has been associated with endocytosis, cytokinesis, cell-to-cell coupling and gating at plasmodesmata. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. It also contains IQ domains Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276834  Cd Length: 647  Bit Score: 620.10  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQyeNPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd01383      2 SVLHNLEYRYSQDIIYTKAGPVLIAVNPFKDVPLYGNEFITAYRQKLL--DSPHVYAVADTAYREMMRDEINQSIIISGE 79
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVQhvkDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNFL 191
Cdd:cd01383     80 SGAGKTETAKIAMQYLAALGGGSSGIE---NEILQTNPILEAFGNAKTLRNDNSSRFGKLIDIHFDAAGKICGAKIQTYL 156
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  192 LEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSIQQ 271
Cdd:cd01383    157 LEKSRVVQLANGERSYHIFYQLCAGASPALREKLNLKSASEYKYLNQSNCLTIDGVDDAKKFHELKEALDTVGISKEDQE 236
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  272 LVLQLVAGILHLGNISFCEDGNYARVESV--DLLAFPAYLLGIDSGRLQEKLTSRKMdsRWGGrsESIDVTLNVEQAAYT 349
Cdd:cd01383    237 HIFQMLAAVLWLGNISFQVIDNENHVEVVadEAVSTAASLLGCNANDLMLALSTRKI--QAGG--DKIVKKLTLQQAIDA 312
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  350 RDALAKGLYARLFDFLVEAINRAMQ--KPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYV 427
Cdd:cd01383    313 RDALAKAIYASLFDWLVEQINKSLEvgKRRTGRSISILDIYGFESFQKNSFEQLCINYANERLQQHFNRHLFKLEQEEYE 392
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  428 QEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNSWSAG-FVIHHYA 506
Cdd:cd01383    393 LDGIDWTKVDFEDNQECLDLIEKK--PLGLISLLDEESNFPKAT----DLTFANKLKQHLKSNSCFKGERGGaFTIRHYA 466
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  507 GKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKKGRPSTA-----------GSKIKKQANDLVATLM 575
Cdd:cd01383    467 GEVTYDTSGFLEKNRDLLHSDLIQLLSSCSCQLPQLFASKMLDASRKALPLTKasgsdsqkqsvATKFKGQLFKLMQRLE 546
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  576 RCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRwRGDERQGVQH 655
Cdd:cd01383    547 NTTPHFIRCIKPNNKQLPGVFDQDLVLQQLRCCGVLEVVRISRSGYPTRMTHQEFARRYGFLLPEDVSA-SQDPLSTSVA 625
                          650       660
                   ....*....|....*....|..
gi 1622892340  656 LLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd01383    626 ILQQFNILPEMYQVGYTKLFFR 647
MYSc_Myo4 cd14872
class IV myosin, motor domain; These myosins all possess a WW domain either N-terminal or ...
32-674 0e+00

class IV myosin, motor domain; These myosins all possess a WW domain either N-terminal or C-terminal to their motor domain and a tail with a MyTH4 domain followed by a SH3 domain in some instances. The monomeric Acanthamoebas were the first identified members of this group and have been joined by Stramenopiles. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276839  Cd Length: 644  Bit Score: 612.55  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14872      2 MIVHNLRKRFKNDQIYTNVGTILISVNPFKRLPLYTPTVMDQYMHKGPKEMPPHTYNIADDAYRAMIVDAMNQSILISGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVQHVkdiILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNFL 191
Cdd:cd14872     82 SGAGKTEATKQCLSFFAEVAGSTNGVEQR---VLLANPILEAFGNAKTLRNNNSSRFGKWVEIHFDNRGRICGASTENYL 158
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  192 LEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPdyYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSIQQ 271
Cdd:cd14872    159 LEKSRVVYQIKGERNFHIFYQLLASPDPASRGGWGSSAA--YGYLSLSGCIEVEGVDDVADFEEVVLAMEQLGFDDADIN 236
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  272 LVLQLVAGILHLGNISFCEDGNYARVESV-----DLLAFPAYLLGIDSGRLQEKLTSRKMDSRwGGRSESIdvTLNVEQA 346
Cdd:cd14872    237 NVMSLIAAILKLGNIEFASGGGKSLVSGStvanrDVLKEVATLLGVDAATLEEALTSRLMEIK-GCDPTRI--PLTPAQA 313
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  347 AYTRDALAKGLYARLFDFLVEAINRAM--QKPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQE 424
Cdd:cd14872    314 TDACDALAKAAYSRLFDWLVKKINESMrpQKGAKTTFIGVLDIFGFEIFEKNSFEQLCINFTNEKLQQHFNQYTFKLEEA 393
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  425 EYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCatmhATGGGADQTLLQKLQAAVGTHEHFNSWSAG----- 499
Cdd:cd14872    394 LYQSEGVKFEHIDFIDNQPVLDLIEKK--QPGLMLALDDQV----KIPKGSDATFMIAANQTHAAKSTFVYAEVRtsrte 467
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  500 FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPeKLDGDKKGRPSTAGSKIKKQANDLVATLMRCTP 579
Cdd:cd14872    468 FIVKHYAGDVTYDITGFLEKNKDTLQKDLYVLLSSSKNKLIAVLFP-PSEGDQKTSKVTLGGQFRKQLSALMTALNATEP 546
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  580 HYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWRGDERQGVQHLLRA 659
Cdd:cd14872    547 HYIRCVKPNQEKRARLFDGFMSLEQLRYAGVFEAVKIRKTGYPFRYSHERFLKRYRFLVKTIAKRVGPDDRQRCDLLLKS 626
                          650
                   ....*....|....*
gi 1622892340  660 VNMEPDQYQMGSTKV 674
Cdd:cd14872    627 LKQDFSKVQVGKTRV 641
MYSc_Myo40 cd14901
class XL myosin, motor domain; The class XL myosins are comprised of Stramenopiles. Not much ...
32-676 0e+00

class XL myosin, motor domain; The class XL myosins are comprised of Stramenopiles. Not much is known about this myosin class. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276866 [Multi-domain]  Cd Length: 655  Bit Score: 575.97  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLY------QGAAQYENPPHIYALTDNMYRNML----IDC 101
Cdd:cd14901      2 SILHVLRRRFAHGLIYTSTGAILVAINPFRRLPLYDDETKEAYyehgerRAAGERKLPPHVYAVADKAFRAMLfasrGQK 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  102 ENQCVIISGESGAGKTVAAKYIMGYISKVSG----GGNKVQH--VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQ 175
Cdd:cd14901     82 CDQSILVSGESGAGKTETTKIIMNYLASVSSatthGQNATERenVRDRVLESNPILEAFGNARTNRNNNSSRFGKFIRLG 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  176 FSRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTY-QVDGTDDRSDFG 254
Cdd:cd14901    162 FASSGSLLGASISTYLLERVRLVSQAKGERNYHIFYELLRGASSDELHALGLTHVEEYKYLNSSQCYdRRDGVDDSVQYA 241
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  255 ETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISFCE---DGNYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMdsRWG 331
Cdd:cd14901    242 KTRHAMTTIGMSPDEQISVLQLVAAVLHLGNLCFVKkdgEGGTFSMSSLANVRAACDLLGLDMDVLEKTLCTREI--RAG 319
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  332 GrsESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAM---QKPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNE 408
Cdd:cd14901    320 G--EYITMPLSVEQALLTRDVVAKTLYAQLFDWLVDRINESIaysESTGASRFIGIVDIFGFEIFATNSLEQLCINFANE 397
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  409 KLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHatggGADQTLLQKLQAAVG 488
Cdd:cd14901    398 KLQQLFGKFVFEMEQDEYVAEAIPWTFVEYPNNDACVAMFEAR--PTGLFSLLDEQCLLPR----GNDEKLANKYYDLLA 471
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  489 THEHFNS-----WSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLrmlfpekldgdkkgrPSTAGSKI 563
Cdd:cd14901    472 KHASFSVsklqqGKRQFVIHHYAGAVCYATDGFCDKNKDHVHSEALALLRTSSNAFL---------------SSTVVAKF 536
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  564 KKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPE--- 640
Cdd:cd14901    537 KVQLSSLLEVLNATEPHFIRCIKPNDVLSPSEFDAKRVLEQLRCSGVLEAVKISRSGYPVRFPHDAFVHTYSCLAPDgas 616
                          650       660       670
                   ....*....|....*....|....*....|....*...
gi 1622892340  641 -TWPRWRGDERQGVQHLLRAVNME-PDQYQMGSTKVFV 676
Cdd:cd14901    617 dTWKVNELAERLMSQLQHSELNIEhLPPFQVGKTKVFL 654
MYSc_Myo29 cd14890
class XXIX myosin, motor domain; Class XXIX myosins are comprised of Stramenopiles and have ...
36-677 0e+00

class XXIX myosin, motor domain; Class XXIX myosins are comprised of Stramenopiles and have very long tail domains consisting of three IQ motifs, short coiled-coil regions, up to 18 CBS domains, a PB1 domain, and a carboxy-terminal transmembrane domain. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276855 [Multi-domain]  Cd Length: 662  Bit Score: 575.96  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMDDYIFTYIGSVLISVNPFKQMP-YFTDREIDLYQGAAQYENPPHIYALTDNMY----RNMLIDCENQCVIISG 110
Cdd:cd14890      6 TLRLRYERDEIYTYVGPILISINPYKSIPdLYSEERMLLYHGTTAGELPPHVFAIADHAYtqliQSGVLDPSNQSIIISG 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  111 ESGAGKTVAAKYIMGYISKVSGGGNKV-------------QHVKDI---ILQSNPLLEAFGNAKTVRNNNSSRFGKYFEI 174
Cdd:cd14890     86 ESGAGKTEATKIIMQYLARITSGFAQGasgegeaaseaieQTLGSLedrVLSSNPLLESFGNAKTLRNDNSSRFGKFIEI 165
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  175 QFSRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLnQSDTYQVDGTDDRSDFG 254
Cdd:cd14890    166 QFDHHGKIVGAEISNFLLEKTRIVTQNDGERNYHIFYQLLAGADEALRERLKLQTPVEYFYL-RGECSSIPSCDDAKAFA 244
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  255 ETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISF--CEDGNYARVE-SVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwg 331
Cdd:cd14890    245 ETIRCLSTIGISEENQDAVFGLLAAVLHLGNVDFesENDTTVLEDAtTLQSLKLAAELLGVNEDALEKALLTRQLFV--- 321
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  332 gRSESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEY-SIGVLDIYGFEIFQKNGFEQFCINFVNEKL 410
Cdd:cd14890    322 -GGKTIVQPQNVEQARDKRDALAKALYSSLFLWLVSELNRTISSPDDKWgFIGVLDIYGFEKFEWNTFEQLCINYANEKL 400
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  411 QQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKLS-PPGIMSVLDDVCATmhaTGGGADQTLLQKLQAAVGT 489
Cdd:cd14890    401 QRHFNQHMFEVEQVEYSNEGIDWQYITFNDNQACLELIEGKVNgKPGIFITLDDCWRF---KGEEANKKFVSQLHASFGR 477
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  490 -------------HEHFNSWSAG----FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFlrmlfpekldgdk 552
Cdd:cd14890    478 ksgsggtrrgssqHPHFVHPKFDadkqFGIKHYAGDVIYDASGFNEKNNETLNAEMKELIKQSRRSI------------- 544
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  553 kgRPSTAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQ 632
Cdd:cd14890    545 --REVSVGAQFRTQLQELMAKISLTNPRYVRCIKPNETKAPGKFDGLDCLRQLKYSGMMEAIQIRQQGFALREEHDSFFY 622
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|....*
gi 1622892340  633 RYAILTPETwprwrGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14890    623 DFQVLLPTA-----ENIEQLVAVLSKMLGLGKADWQIGSSKIFLK 662
MYSc_Myo9 cd01385
class IX myosin, motor domain; Myosin IX is a processive single-headed motor, which might play ...
36-677 0e+00

class IX myosin, motor domain; Myosin IX is a processive single-headed motor, which might play a role in signalling. It has a N-terminal RA domain, an IQ domain, a C1_1 domain, and a RhoGAP domain. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276836 [Multi-domain]  Cd Length: 690  Bit Score: 567.39  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGAG 115
Cdd:cd01385      6 NLRARFKHGKIYTYVGSILIAVNPFKFLPIYNPKYVKMYQNRRLGKLPPHIFAIADVAYHAMLRKKKNQCIVISGESGSG 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  116 KTVAAKYIMGYISKVS--GGGNKVQHvkdIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNFLLE 193
Cdd:cd01385     86 KTESTNFLLHHLTALSqkGYGSGVEQ---TILGAGPVLEAFGNAKTAHNNNSSRFGKFIQVNYRENGMVRGAVVEKYLLE 162
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  194 KSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSIQQLV 273
Cdd:cd01385    163 KSRIVSQEKNERNYHVFYYLLAGASEEERKELHLKQPEDYHYLNQSDCYTLEGEDEKYEFERLKQAMEMVGFLPETQRQI 242
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  274 LQLVAGILHLGNISFCEDGNY----ARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNVEQAAYT 349
Cdd:cd01385    243 FSVLSAVLHLGNIEYKKKAYHrdesVTVGNPEVLDIISELLRVKEETLLEALTTKKTVT----VGETLILPYKLPEAIAT 318
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  350 RDALAKGLYARLFDFLVEAINRAMQKPQEE-----YSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQE 424
Cdd:cd01385    319 RDAMAKCLYSALFDWIVLRINHALLNKKDLeeakgLSIGVLDIFGFEDFGNNSFEQFCINYANEHLQYYFNQHIFKLEQE 398
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  425 EYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNS---WSAGFV 501
Cdd:cd01385    399 EYKKEGISWHNIEYTDNTGCLQLISKK--PTGLLCLLDEESNFPGAT----NQTLLAKFKQQHKDNKYYEKpqvMEPAFI 472
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  502 IHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRML-----------------------FPEK----------- 547
Cdd:cd01385    473 IAHYAGKVKYQIKDFREKNLDLMRPDIVAVLRSSSSAFVRELigidpvavfrwavlrafframaaFREAgrrraqrtagh 552
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  548 ------------LDGDKKGRPSTAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIR 615
Cdd:cd01385    553 sltlhdrttkslLHLHKKKKPPSVSAQFQTSLSKLMETLGQAEPFFIRCIKSNAEKKPLRFDDELVLRQLRYTGMLETVR 632
                          650       660       670       680       690       700
                   ....*....|....*....|....*....|....*....|....*....|....*....|..
gi 1622892340  616 VRRAGFAYRRQFAKFLQRYAILTpetwPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd01385    633 IRRSGYSVRYTFQEFITQFQVLL----PKGLISSKEDIKDFLEKLNLDRDNYQIGKTKVFLK 690
MYSc_Myo6 cd01382
class VI myosin, motor domain; Myosin VI is a monomeric myosin, which moves towards the ...
36-675 0e+00

class VI myosin, motor domain; Myosin VI is a monomeric myosin, which moves towards the minus-end of actin filaments, in contrast to most other myosins which moves towards the plus-end of actin filaments. It is thought that myosin VI, unlike plus-end directed myosins, does not use a pure lever arm mechanism, but instead steps with a mechanism analogous to the kinesin neck-linker uncoupling model. It has been implicated in a myriad of functions including: the transport of cytoplasmic organelles, maintenance of normal Golgi morphology, endocytosis, secretion, cell migration, border cell migration during development, and in cancer metastasis playing roles in deafness and retinal development among others. While how this is accomplished is largely unknown there are several interacting proteins that have been identified such as disabled homolog 2 (DAB2), GIPC1, synapse-associated protein 97 (SAP97; also known as DLG1) and optineurin, which have been found to target myosin VI to different cellular compartments. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the minus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276833  Cd Length: 649  Bit Score: 555.71  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDRE-IDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGA 114
Cdd:cd01382      6 NIRVRYSKDKIYTYVANILIAVNPYFDIPKLYSSEtIKSYQGKSLGTLPPHVFAIADKAYRDMKVLKQSQSIIVSGESGA 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  115 GKTVAAKYIMGYIskVSGGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNFLLEK 194
Cdd:cd01382     86 GKTESTKYILRYL--TESWGSGAGPIEQRILEANPLLEAFGNAKTVRNNNSSRFGKFVEIHFNEKSSVVGGFVSHYLLEK 163
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  195 SRVVMQNENERNFHIYYQLLEGASQEQRQNLglmtpdyyyylnqsdtyQVDGT-DDRSDFGETLSAMQVIGIPPSIQQLV 273
Cdd:cd01382    164 SRICVQSKEERNYHIFYRLCAGAPEDLREKL-----------------LKDPLlDDVGDFIRMDKAMKKIGLSDEEKLDI 226
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  274 LQLVAGILHLGNISFCEDGNYARV------ESVDLLAFPAYLLGIDSGRLQEKLTSRKMD-SRWGGRSESIDVTLNVEQA 346
Cdd:cd01382    227 FRVVAAVLHLGNIEFEENGSDSGGgcnvkpKSEQSLEYAAELLGLDQDELRVSLTTRVMQtTRGGAKGTVIKVPLKVEEA 306
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  347 AYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEY 426
Cdd:cd01382    307 NNARDALAKAIYSKLFDHIVNRINQCIPFETSSYFIGVLDIAGFEYFEVNSFEQFCINYCNEKLQQFFNERILKEEQELY 386
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  427 VQEGIRWTPIQYFNNKVVCDLIENKLSppGIMSVLDDVCatmhatgggadqtllqKLQAAvgTHEHF-----NSW----- 496
Cdd:cd01382    387 EKEGLGVKEVEYVDNQDCIDLIEAKLV--GILDLLDEES----------------KLPKP--SDQHFtsavhQKHknhfr 446
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  497 -----------------SAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKKGRPSTA 559
Cdd:cd01382    447 lsiprksklkihrnlrdDEGFLIRHFAGAVCYETAQFIEKNNDALHASLESLICESKDKFIRSLFESSTNNNKDSKQKAG 526
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  560 -------GSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQ 632
Cdd:cd01382    527 klsfisvGNKFKTQLNLLMDKLRSTGTSFIRCIKPNLKMTSHHFEGAQILSQLQCSGMVSVLDLMQGGFPSRTSFHDLYN 606
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|...
gi 1622892340  633 RYAILTPETWPRWrgDERQGVQHLLRAVNMEPDQYQMGSTKVF 675
Cdd:cd01382    607 MYKKYLPPKLARL--DPRLFCKALFKALGLNENDFKFGLTKVF 647
MYSc_Myo10 cd14873
class X myosin, motor domain; Myosin X is an unconventional myosin motor that functions as a ...
32-677 0e+00

class X myosin, motor domain; Myosin X is an unconventional myosin motor that functions as a monomer. In mammalian cells, the motor is found to localize to filopodia. Myosin X walks towards the barbed ends of filaments and is thought to walk on bundles of actin, rather than single filaments, a unique behavior. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. C-terminal to the head domain are a variable number of IQ domains, 2 PH domains, a MyTH4 domain, and a FERM domain. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276840 [Multi-domain]  Cd Length: 651  Bit Score: 550.55  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDRE-IDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISG 110
Cdd:cd14873      2 SIMYNLFQRYKRNQIYTYIGSILASVNPYQPIAGLYEPAtMEQYSRRHLGELPPHIFAIANECYRCLWKRHDNQCILISG 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  111 ESGAGKTVAAKYIMGYISKVS------GGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDG 184
Cdd:cd14873     82 ESGAGKTESTKLILKFLSVISqqslelSLKEKTSCVEQAILESSPIMEAFGNAKTVYNNNSSRFGKFVQLNICQKGNIQG 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  185 GKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIG 264
Cdd:cd14873    162 GRIVDYLLEKNRVVRQNPGERNYHIFYALLAGLEHEEREEFYLSTPENYHYLNQSGCVEDKTISDQESFREVITAMEVMQ 241
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  265 IPPSIQQLVLQLVAGILHLGNISFCEDGNyARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNVE 344
Cdd:cd14873    242 FSKEEVREVSRLLAGILHLGNIEFITAGG-AQVSFKTALGRSAELLGLDPTQLTDALTQRSMFL----RGEEILTPLNVQ 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  345 QAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQE 424
Cdd:cd14873    317 QAVDSRDSLAMALYARCFEWVIKKINSRIKGKEDFKSIGILDIFGFENFEVNHFEQFNINYANEKLQEYFNKHIFSLEQL 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  425 EYVQEGIRWTPIQYFNNKVVCDLIENKLsppGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHF---NSWSAGFV 501
Cdd:cd14873    397 EYSREGLVWEDIDWIDNGECLDLIEKKL---GLLALINEESHFPQAT----DSTLLEKLHSQHANNHFYvkpRVAVNNFG 469
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  502 IHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP--------EKLDGDKKGRPSTAGSKIKKQANDLVAT 573
Cdd:cd14873    470 VKHYAGEVQYDVRGILEKNRDTFRDDLLNLLRESRFDFIYDLFEhvssrnnqDTLKCGSKHRRPTVSSQFKDSLHSLMAT 549
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  574 LMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPE-TWPRwrgDERQG 652
Cdd:cd14873    550 LSSSNPFFVRCIKPNMQKMPDQFDQAVVLNQLRYSGMLETVRIRKAGYAVRRPFQDFYKRYKVLMRNlALPE---DVRGK 626
                          650       660
                   ....*....|....*....|....*
gi 1622892340  653 VQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14873    627 CTSLLQLYDASNSEWQLGKTKVFLR 651
MYSc_Myo3 cd01379
class III myosin, motor domain; Myosin III has been shown to play a role in the vision process ...
31-677 0e+00

class III myosin, motor domain; Myosin III has been shown to play a role in the vision process in insects and in hearing in mammals. Myosin III, an unconventional myosin, does not form dimers. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. They are characterized by an N-terminal protein kinase domain and several IQ domains. Some members also contain WW, SH2, PH, and Y-phosphatase domains. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276830 [Multi-domain]  Cd Length: 633  Bit Score: 543.41  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   31 DAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISG 110
Cdd:cd01379      1 DTIVSQLQKRYSRDQIYTYIGDILIAVNPFQNLGIYTEEHSRLYRGAKRSDNPPHIFAVADAAYQAMIHQKKNQCIVISG 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  111 ESGAGKTVAAKYIMGYISKVSGGGNkvQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNF 190
Cdd:cd01379     81 ESGAGKTESANLLVQQLTVLGKANN--RTLEEKILQVNPLMEAFGNARTVINDNSSRFGKYLEMKFTSTGAVTGARISEY 158
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  191 LLEKSRVVMQNENERNFHIYYQLLEG-ASQEQRQNLGL-MTPDYYYYLNQSDTYQvDGTDD---RSDFGETLSAMQVIGI 265
Cdd:cd01379    159 LLEKSRVVHQAIGERNFHIFYYIYAGlAEDKKLAKYKLpENKPPRYLQNDGLTVQ-DIVNNsgnREKFEEIEQCFKVIGF 237
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  266 PPSIQQLVLQLVAGILHLGNISFCEDG------NYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDV 339
Cdd:cd01379    238 TKEEVDSVYSILAAILHIGDIEFTEVEsnhqtdKSSRISNPEALNNVAKLLGIEADELQEALTSHSVVT----RGETIIR 313
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  340 TLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQ----KPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFI 415
Cdd:cd01379    314 NNTVEEATDARDAMAKALYGRLFSWIVNRINSLLKpdrsASDEPLSIGILDIFGFENFQKNSFEQLCINIANEQIQYYFN 393
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  416 ELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHF-- 493
Cdd:cd01379    394 QHIFAWEQQEYLNEGIDVDLIEYEDNRPLLDMFLQK--PMGLLALLDEESRFPKAT----DQTLVEKFHNNIKSKYYWrp 467
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  494 NSWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMlfpekldgdkkgrpsTAGSKIKKQANDLVAT 573
Cdd:cd01379    468 KSNALSFGIHHYAGKVLYDASGFLEKNRDTLPPDVVQLLRSSENPLVRQ---------------TVATYFRYSLMDLLSK 532
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  574 LMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTpetwprWRGDE---- 649
Cdd:cd01379    533 MVVGQPHFVRCIKPNDSRQAGKFDREKVLKQLRYTGVLETTRIRRQGFSHRILFADFLKRYYFLA------FKWNEevva 606
                          650       660
                   ....*....|....*....|....*....
gi 1622892340  650 -RQGVQHLLRAVNMepDQYQMGSTKVFVK 677
Cdd:cd01379    607 nRENCRLILERLKL--DNWALGKTKVFLK 633
MYSc_Myo46 cd14907
class XLVI myosin, motor domain; The class XLVI myosins are comprised of Alveolata. Not much ...
36-637 1.28e-177

class XLVI myosin, motor domain; The class XLVI myosins are comprised of Alveolata. Not much is known about this myosin class. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276872 [Multi-domain]  Cd Length: 669  Bit Score: 536.54  E-value: 1.28e-177
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMDDYIFTYIGSVLISVNPFKQMPY-FTDREIDLYQGAA--------QYENPPHIYALTDNMYRNMLIDCENQCV 106
Cdd:cd14907      6 NLKKRYQQDKIFTYVGPTLIVMNPYKQIDNlFSEEVMQMYKEQIiqngeyfdIKKEPPHIYAIAALAFKQLFENNKKQAI 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  107 IISGESGAGKTVAAKYIMGYISKVSG-----------------GGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFG 169
Cdd:cd14907     86 VISGESGAGKTENAKYAMKFLTQLSQqeqnseevltltssiraTSKSTKSIEQKILSCNPILEAFGNAKTVRNDNSSRFG 165
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  170 KYFEIQFS-RGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDY---YYYLNQSDTYQVD 245
Cdd:cd14907    166 KYVSILVDkKKRKILGARIQNYLLEKSRVTQQGQGERNYHIFYHLLYGADQQLLQQLGLKNQLSgdrYDYLKKSNCYEVD 245
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  246 GTDDRSDFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISFCE----DGNYARVESVDLLAFPAYLLGIDSGRLQEKL 321
Cdd:cd14907    246 TINDEKLFKEVQQSFQTLGFTEEEQDSIWRILAAILLLGNLQFDDstldDNSPCCVKNKETLQIIAKLLGIDEEELKEAL 325
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  322 TSRKmdSRWGGrsESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAM--------QKPQEEY-SIGVLDIYGFEI 392
Cdd:cd14907    326 TTKI--RKVGN--QVITSPLSKKECINNRDSLSKELYDRLFNWLVERLNDTImpkdekdqQLFQNKYlSIGLLDIFGFEV 401
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  393 FQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQEGI--RWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCatmhA 470
Cdd:cd14907    402 FQNNSFEQLCINYTNEKLQQLYISYVFKAEEQEFKEEGLedYLNQLSYTDNQDVIDLLDKP--PIGIFNLLDDSC----K 475
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  471 TGGGADQTLLQKLQAAVGTHEHFNSWSAG----FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPE 546
Cdd:cd14907    476 LATGTDEKLLNKIKKQHKNNSKLIFPNKInkdtFTIRHTAKEVEYNIEGFREKNKDEISQSIINCIQNSKNRIISSIFSG 555
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  547 KLDGDKKGRPSTA---------GSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVR 617
Cdd:cd14907    556 EDGSQQQNQSKQKksqkkdkflGSKFRNQMKQLMNELMQCDVHFIRCIKPNEEKKADLFIQGYVLNQIRYLGVLESIRVR 635
                          650       660
                   ....*....|....*....|
gi 1622892340  618 RAGFAYRRQFAKFLQRYAIL 637
Cdd:cd14907    636 KQGYPYRKSYEDFYKQYSLL 655
MYSc_Myo31 cd14892
class XXXI myosin, motor domain; Class XXXI myosins have a very long neck region consisting of ...
37-677 1.02e-176

class XXXI myosin, motor domain; Class XXXI myosins have a very long neck region consisting of 17 IQ motifs and 2 tandem ANK repeats that are separated by a PH domain. The myosin classes XXX to XXXIV contain members from Phytophthora species and Hyaloperonospora parasitica. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276857 [Multi-domain]  Cd Length: 656  Bit Score: 533.57  E-value: 1.02e-176
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   37 LRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDreIDLYQGAAQYEN-----PPHIYALTDNMYRNMLID----CENQCVI 107
Cdd:cd14892      7 LRRRYERDAIYTFTADILISINPYKSIPLLYD--VPGFDSQRKEEAtasspPPHVFSIAERAYRAMKGVgkgqGTPQSIV 84
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  108 ISGESGAGKTVAAKYIMGYISKVSGGGNKV----------QHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFS 177
Cdd:cd14892     85 VSGESGAGKTEASKYIMKYLATASKLAKGAstskgaanahESIEECVLLSNLILEAFGNAKTIRNDNSSRFGKYIQIHYN 164
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  178 RGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETL 257
Cdd:cd14892    165 SDGRIAGASTDHFLLEKSRLVGPDANERNYHIFYQLLAGLDANENAALELTPAESFLFLNQGNCVEVDGVDDATEFKQLR 244
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  258 SAMQVIGIPPSIQQLVLQLVAGILHLGNISFCE----DGNYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDsrwGGR 333
Cdd:cd14892    245 DAMEQLGFDAEFQRPIFEVLAAVLHLGNVRFEEnaddEDVFAQSADGVNVAKAAGLLGVDAAELMFKLVTQTTS---TAR 321
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  334 SESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQ-----------KPQEEYSIGVLDIYGFEIFQKNGFEQFC 402
Cdd:cd14892    322 GSVLEIKLTAREAKNALDALCKYLYGELFDWLISRINACHKqqtsgvtggaaSPTFSPFIGILDIFGFEIMPTNSFEQLC 401
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  403 INFVNEKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggADQTLLQK 482
Cdd:cd14892    402 INFTNEMLQQQFNKHVFVLEQEVYASEGIDVSAIEFQDNQDCLDLIQKK--PLGLLPLLEEQMLLKRKT---TDKQLLTI 476
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  483 L-QAAVGTHEHFNSWSAG---FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSeqaflrmlfpekldgdkkgrpst 558
Cdd:cd14892    477 YhQTHLDKHPHYAKPRFEcdeFVLRHYAGDVTYDVHGFLAKNNDNLHDDLRDLLRSS----------------------- 533
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  559 agSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILT 638
Cdd:cd14892    534 --SKFRTQLAELMEVLWSTTPSYIKCIKPNNLKFPGGFSCELVRDQLIYSGVLEVVRIRREGFPIRRQFEEFYEKFWPLA 611
                          650       660       670       680       690
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340  639 petwpRWR----GDERQGVQHLLR-------AVNMEPDQYQMGSTKVFVK 677
Cdd:cd14892    612 -----RNKagvaASPDACDATTARkkceeivARALERENFQLGRTKVFLR 656
MYSc_Myo15 cd01387
class XV mammal-like myosin, motor domain; The class XV myosins are monomeric. In vertebrates, ...
32-677 2.13e-176

class XV mammal-like myosin, motor domain; The class XV myosins are monomeric. In vertebrates, myosin XV appears to be expressed in sensory tissue and play a role in hearing. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. C-terminal to the head domain are 2 MyTH4 domain, a FERM domain, and a SH3 domain. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276838 [Multi-domain]  Cd Length: 657  Bit Score: 532.79  E-value: 2.13e-176
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd01387      2 TVLWNLKTRYERNLIYTYIGSILVSVNPYKMFDIYGLEQVQQYSGRALGELPPHLFAIANLAFAKMLDAKQNQCVVISGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVqhVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFsRGGEPDGGKISNFL 191
Cdd:cd01387     82 SGSGKTEATKLIMQYLAAVNQRRNNL--VTEQILEATPLLEAFGNAKTVRNDNSSRFGKYLEVFF-EGGVIVGAITSQYL 158
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  192 LEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSIQQ 271
Cdd:cd01387    159 LEKSRIVTQAKNERNYHVFYELLAGLPAQLRQKYGLQEAEKYFYLNQGGNCEIAGKSDADDFRRLLAAMQVLGFSSEEQD 238
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  272 LVLQLVAGILHLGNISFCEDGNYARVESVDL-----LAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNVEQA 346
Cdd:cd01387    239 SIFRILASVLHLGNVYFHKRQLRHGQEGVSVgsdaeIQWVAHLLQISPEGLQKALTFKVTET----RRERIFTPLTIDQA 314
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  347 AYTRDALAKGLYARLFDFLVEAINRAMQKP-QEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEE 425
Cdd:cd01387    315 LDARDAIAKALYALLFSWLVTRVNAIVYSGtQDTLSIAILDIFGFEDLSENSFEQLCINYANENLQYYFNKHVFKLEQEE 394
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  426 YVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNSWSAG---FVI 502
Cdd:cd01387    395 YIREQIDWTEIAFADNQPVINLISKK--PVGILHILDDECNFPQAT----DHSFLEKCHYHHALNELYSKPRMPlpeFTI 468
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  503 HHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLF-----------PEKLDG---DKKGRPSTAGSKIKKQAN 568
Cdd:cd01387    469 KHYAGQVWYQVHGFLDKNRDQLRQDVLELLVSSRTRVVAHLFsshraqtdkapPRLGKGrfvTMKPRTPTVAARFQDSLL 548
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  569 DLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWR-G 647
Cdd:cd01387    549 QLLEKMERCNPWFVRCLKPNHKKEPMLFDMDVVMAQLRYSGMLETIRIRKEGYPVRLPFQVFIDRYRCLVALKLPRPApG 628
                          650       660       670
                   ....*....|....*....|....*....|
gi 1622892340  648 DERQGVQHLLRAVNMEPDqYQMGSTKVFVK 677
Cdd:cd01387    629 DMCVSLLSRLCTVTPKDM-YRLGATKVFLR 657
MYSc_Myo42 cd14903
class XLII myosin, motor domain; The class XLII myosins are comprised of Stramenopiles. Not ...
32-675 7.57e-172

class XLII myosin, motor domain; The class XLII myosins are comprised of Stramenopiles. Not much is known about this myosin class. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276868 [Multi-domain]  Cd Length: 658  Bit Score: 520.87  E-value: 7.57e-172
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDL-YQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISG 110
Cdd:cd14903      2 AILYNVKKRFLRKLPYTYTGDICIAVNPYQWLPELYTEEQHSkYLNKPKEELPPHVYATSVAAYNHMKRSGRNQSILVSG 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  111 ESGAGKTVAAKYIMGYISKVSGGGNKVQhVKDIIlQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNF 190
Cdd:cd14903     82 ESGAGKTETTKILMNHLATIAGGLNDST-IKKII-EVNPLLESFGNAKTVRNDNSSRFGKFTQLQFDKNGTLVGAKCRTY 159
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  191 LLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGlmTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSIQ 270
Cdd:cd14903    160 LLEKTRVISHERPERNYHIFYQLLASPDVEERLFLD--SANECAYTGANKTIKIEGMSDRKHFARTKEALSLIGVSEEKQ 237
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  271 QLVLQLVAGILHLGNISFCEDGNYARVESVDL----LAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNVEQA 346
Cdd:cd14903    238 EVLFEVLAGILHLGQLQIQSKPNDDEKSAIAPgdqgAVYATKLLGLSPEALEKALCSRTMRA----AGDVYTVPLKKDQA 313
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  347 AYTRDALAKGLYARLFDFLVEAINRAMQ-KPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEE 425
Cdd:cd14903    314 EDCRDALAKAIYSNVFDWLVATINASLGnDAKMANHIGVLDIFGFEHFKHNSFEQFCINYANEKLQQKFTQDVFKTVQIE 393
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  426 YVQEGIRWTPIQYFNNKVVCDLIENKLsppGIMSVLDDvcATMHATGGgaDQTLLQKLQAAVGTHEH---FNSWS-AGFV 501
Cdd:cd14903    394 YEEEGIRWAHIDFADNQDVLAVIEDRL---GIISLLND--EVMRPKGN--EESFVSKLSSIHKDEQDvieFPRTSrTQFT 466
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  502 IHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLD-------------GDKKGRP---STAGSKIKK 565
Cdd:cd14903    467 IKHYAGPVTYESLGFLEKHKDALLPDLSDLMRGSSKPFLRMLFKEKVEspaaastslargaRRRRGGAlttTTVGTQFKD 546
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  566 QANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETwPRW 645
Cdd:cd14903    547 SLNELMTTIRSTNVHYVRCIKPNSIKSPTELDHLMVVSQLRCAGVIEAIRISRAAYPNRLLHEEFLDKFWLFLPEG-RNT 625
                          650       660       670
                   ....*....|....*....|....*....|.
gi 1622892340  646 RGDERQGVQHLLRAVNME-PDQYQMGSTKVF 675
Cdd:cd14903    626 DVPVAERCEALMKKLKLEsPEQYQMGLTRIY 656
MYSc_Myo36 cd14897
class XXXVI myosin, motor domain; This class of molluscan myosins contains a motor domain ...
33-677 8.50e-172

class XXXVI myosin, motor domain; This class of molluscan myosins contains a motor domain followed by a GlcAT-I (Beta1,3-glucuronyltransferase I) domain. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276862 [Multi-domain]  Cd Length: 635  Bit Score: 520.02  E-value: 8.50e-172
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   33 IAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQG-AAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14897      3 IVQTLKSRYNKDKFYTYIGDILVAVNPCKPLPIFDKKHHEEYSNlSVRSQRPPHLFWIADQAYRRLLETGRNQCILVSGE 82
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVQHVKdiILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNFL 191
Cdd:cd14897     83 SGAGKTESTKYMIKHLMKLSPSDDSDLLDK--IVQINPLLEAFGNASTVMNDNSSRFGKFIELHFTENGQLLGAKIDDYL 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  192 LEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDD------RSDFGETLSAMQVIGI 265
Cdd:cd14897    161 LEKSRVVHRGNGEKNFHIFYALFAGMSRDRLLYYFLEDPDCHRILRDDNRNRPVFNDSeeleyyRQMFHDLTNIMKLIGF 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  266 PPSIQQLVLQLVAGILHLGNISF--CEDGNYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNV 343
Cdd:cd14897    241 SEEDISVIFTILAAILHLTNIVFipDEDTDGVTVADEYPLHAVAKLLGIDEVELTEALISNVNTI----RGERIQSWKSL 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  344 EQAAYTRDALAKGLYARLFDFLVEAINRAMqKPQEEY-------SIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIE 416
Cdd:cd14897    317 RQANDSRDALAKDLYSRLFGWIVGQINRNL-WPDKDFqimtrgpSIGILDMSGFENFKINSFDQLCINLSNERLQQYFND 395
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  417 LTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNSW 496
Cdd:cd14897    396 YVFPRERSEYEIEGIEWRDIEYHDNDDVLELFFKK--PLGILPLLDEESTFPQST----DSSLVQKLNKYCGESPRYVAS 469
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  497 SAG---FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPekldgdkkgrpstagSKIKKQANDLVAT 573
Cdd:cd14897    470 PGNrvaFGIRHYAEQVTYDADGFLEKNRDNLSSDIVGCLLNSNNEFISDLFT---------------SYFKRSLSDLMTK 534
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  574 LMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPeTWPRWRGDERQGV 653
Cdd:cd14897    535 LNSADPLFVRCIKPNNFLRPNKFDDELVRRQLLCNGLMEIAKIRRDGYPIRIKYEDFVKRYKEICD-FSNKVRSDDLGKC 613
                          650       660
                   ....*....|....*....|....
gi 1622892340  654 QHLLRAVNMEpdQYQMGSTKVFVK 677
Cdd:cd14897    614 QKILKTAGIK--GYQFGKTKVFLK 635
MYSc_Myo27 cd14888
class XXVII myosin, motor domain; Not much is known about this myosin class. The catalytic ...
32-640 3.24e-168

class XXVII myosin, motor domain; Not much is known about this myosin class. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276853 [Multi-domain]  Cd Length: 667  Bit Score: 511.93  E-value: 3.24e-168
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14888      2 SILHSLNLRFDIDEIYTFTGPILIAVNPFKTIPGLYSDEMLLKFIQPSISKSPHVFSTASSAYQGMCNNKKSQTILISGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKV-SGGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFS--RGGEPD----- 183
Cdd:cd14888     82 SGAGKTESTKYVMKFLACAgSEDIKKRSLVEAQVLESNPLLEAFGNARTLRNDNSSRFGKFIELQFSklKSKRMSgdrgr 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  184 --GGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYY-----------------------YLNQ 238
Cdd:cd14888    162 lcGAKIQTYLLEKVRVCDQQEGERNYHIFYQLCAAAREAKNTGLSYEENDEKLakgadakpisidmssfephlkfrYLTK 241
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  239 SDTYQVDGTDDRSDFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISF-----CEDGNYARVESVDLLAFPAYLLGID 313
Cdd:cd14888    242 SSCHELPDVDDLEEFESTLYAMQTVGISPEEQNQIFSIVAAILYLGNILFenneaCSEGAVVSASCTDDLEKVASLLGVD 321
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  314 SGRLQEKLTSRKMDSRwggrSESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEE--YSIGVLDIYGFE 391
Cdd:cd14888    322 AEDLLNALCYRTIKTA----HEFYTKPLRVDEAEDVRDALARALYSCLFDKVVERTNESIGYSKDNslLFCGVLDIFGFE 397
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  392 IFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCatmhAT 471
Cdd:cd14888    398 CFQLNSFEQLCINFTNERLQQFFNNFVFKCEEKLYIEEGISWNPLDFPDNQDCVDLLQEK--PLGIFCMLDEEC----FV 471
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  472 GGGADQTLLQKLQAAVGTHEHFNSW---SAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKL 548
Cdd:cd14888    472 PGGKDQGLCNKLCQKHKGHKRFDVVktdPNSFVIVHFAGPVKYCSDGFLEKNKDQLSVDAQEVIKNSKNPFISNLFSAYL 551
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  549 D-----GDKKGRPSTAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAY 623
Cdd:cd14888    552 RrgtdgNTKKKKFVTVSSEFRNQLDVLMETIDKTEPHFIRCIKPNSQNVPDLFDRISVNEQLKYGGVLQAVQVSRAGYPV 631
                          650
                   ....*....|....*..
gi 1622892340  624 RRQFAKFLQRYAILTPE 640
Cdd:cd14888    632 RLSHAEFYNDYRILLNG 648
MYSc_Myh10 cd14920
class II myosin heavy chain 10, motor domain; Myosin motor domain of non-muscle myosin heavy ...
36-677 6.72e-157

class II myosin heavy chain 10, motor domain; Myosin motor domain of non-muscle myosin heavy chain 10 (also called NMMHCB). Mutations in this gene have been associated with May-Hegglin anomaly and developmental defects in brain and heart. Multiple transcript variants encoding different isoforms have been found for this gene. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276952 [Multi-domain]  Cd Length: 673  Bit Score: 482.59  E-value: 6.72e-157
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGAG 115
Cdd:cd14920      6 NLKDRYYSGLIYTYSGLFCVVINPYKNLPIYSENIIEMYRGKKRHEMPPHIYAISESAYRCMLQDREDQSILCTGESGAG 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  116 KTVAAKYIMGYISKVSGG------GNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISN 189
Cdd:cd14920     86 KTENTKKVIQYLAHVASShkgrkdHNIPGELERQLLQANPILESFGNAKTVKNDNSSRFGKFIRINFDVTGYIVGANIET 165
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  190 FLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSdTYQVDGTDDRSDFGETLSAMQVIGIPPSI 269
Cdd:cd14920    166 YLLEKSRAVRQAKDERTFHIFYQLLSGAGEHLKSDLLLEGFNNYRFLSNG-YIPIPGQQDKDNFQETMEAMHIMGFSHEE 244
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  270 QQLVLQLVAGILHLGNISFCEDGNYARVESVDLLAFP--AYLLGIDSGRLQEKLTSRKMDSrwgGRsESIDVTLNVEQAA 347
Cdd:cd14920    245 ILSMLKVVSSVLQFGNISFKKERNTDQASMPENTVAQklCHLLGMNVMEFTRAILTPRIKV---GR-DYVQKAQTKEQAD 320
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  348 YTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS--IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEE 425
Cdd:cd14920    321 FAVEALAKATYERLFRWLVHRINKALDRTKRQGAsfIGILDIAGFEIFELNSFEQLCINYTNEKLQQLFNHTMFILEQEE 400
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  426 YVQEGIRWTPIQYFNNKVVC-DLIENKLSPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNSW-----SAG 499
Cdd:cd14920    401 YQREGIEWNFIDFGLDLQPCiDLIERPANPPGVLALLDEECWFPKAT----DKTFVEKLVQEQGSHSKFQKPrqlkdKAD 476
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  500 FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPE-----KLDGD--------------KKGRPSTAG 560
Cdd:cd14920    477 FCIIHYAGKVDYKADEWLMKNMDPLNDNVATLLHQSSDRFVAELWKDvdrivGLDQVtgmtetafgsayktKKGMFRTVG 556
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  561 SKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPE 640
Cdd:cd14920    557 QLYKESLTKLMATLRNTNPNFVRCIIPNHEKRAGKLDPHLVLDQLRCNGVLEGIRICRQGFPNRIVFQEFRQRYEILTPN 636
                          650       660       670
                   ....*....|....*....|....*....|....*..
gi 1622892340  641 TWPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14920    637 AIPKGFMDGKQACERMIRALELDPNLYRIGQSKIFFR 673
MYSc_Myo35 cd14896
class XXXV myosin, motor domain; This class of metazoan myosins contains 2 IQ motifs, 2 MyTH4 ...
36-677 8.01e-157

class XXXV myosin, motor domain; This class of metazoan myosins contains 2 IQ motifs, 2 MyTH4 domains, a single FERM domain, and an SH3 domain. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276861 [Multi-domain]  Cd Length: 644  Bit Score: 481.59  E-value: 8.01e-157
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGAG 115
Cdd:cd14896      6 CLKKRFHLGRIYTFGGPILLSLNPHRSLPLFSEEVLASYHPRKALNTTPHIFAIAASAYRLSQSTGQDQCILLSGHSGSG 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  116 KTVAAKYIMGYISKV--SGGGNKVQHVKDIIlqsnPLLEAFGNAKTVRNNNSSRFGKYFEIQFsRGGEPDGGKISNFLLE 193
Cdd:cd14896     86 KTEAAKKIVQFLSSLyqDQTEDRLRQPEDVL----PILESFGHAKTILNANASRFGQVLRLHL-QHGVIVGASVSHYLLE 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  194 KSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSIQQLV 273
Cdd:cd14896    161 TSRVVFQAQAERSFHVFYELLAGLDPEEREQLSLQGPETYYYLNQGGACRLQGKEDAQDFEGLLKALQGLGLCAEELTAI 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  274 LQLVAGILHLGNISFC----EDGNYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSRWGGRSESidvtLNVEQAAYT 349
Cdd:cd14896    241 WAVLAAILQLGNICFSsserESQEVAAVSSWAEIHTAARLLQVPPERLEGAVTHRVTETPYGRVSRP----LPVEGAIDA 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  350 RDALAKGLYARLFDFLVEAINRAMQKPQEEYS---IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEY 426
Cdd:cd14896    317 RDALAKTLYSRLFTWLLKRINAWLAPPGEAESdatIGVVDAYGFEALRVNGLEQLCINLASERLQLFSSQTLLAQEEEEC 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  427 VQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHehfnSWSAG------- 499
Cdd:cd14896    397 QRELLPWVPIPQPPRESCLDLLVDQ--PHSLLSILDDQTWLSQAT----DHTFLQKCHYHHGDH----PSYAKpqlplpv 466
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  500 FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLD--GDKKGRPsTAGSKIKKQANDLVATLMRC 577
Cdd:cd14896    467 FTVRHYAGTVTYQVHKFLNRNRDQLDPAVVEMLAQSQLQLVGSLFQEAEPqyGLGQGKP-TLASRFQQSLGDLTARLGRS 545
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  578 TPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWRGDERQGVQhLL 657
Cdd:cd14896    546 HVYFIHCLNPNPGKLPGLFDVGHVTEQLRQAGILEAIGTRSEGFPVRVPFQAFLARFGALGSERQEALSDRERCGAI-LS 624
                          650       660
                   ....*....|....*....|
gi 1622892340  658 RAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14896    625 QVLGAESPLYHLGATKVLLK 644
MYSc_Myo43 cd14904
class XLIII myosin, motor domain; The class XLIII myosins are comprised of Stramenopiles. Not ...
32-677 1.55e-156

class XLIII myosin, motor domain; The class XLIII myosins are comprised of Stramenopiles. Not much is known about this myosin class. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276869  Cd Length: 653  Bit Score: 480.98  E-value: 1.55e-156
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMP-YFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISG 110
Cdd:cd14904      2 SILFNLKKRFAASKPYTYTNDIVIALNPYKWIDnLYGDHLHEQYLKKPRDKLQPHVYATSTAAYKHMLTNEMNQSILVSG 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  111 ESGAGKTVAAKYIMGYISKVSGGgnKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNF 190
Cdd:cd14904     82 ESGAGKTETTKIVMNHLASVAGG--RKDKTIAKVIDVNPLLESFGNAKTTRNDNSSRFGKFTQLQFDGRGKLIGAKCETY 159
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  191 LLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQS-DTYQVDGTDDRSDFGETLSAMQVIGIPPSI 269
Cdd:cd14904    160 LLEKSRVVSIAEGERNYHIFYQLLAGLSSEERKEFGLDPNCQYQYLGDSlAQMQIPGLDDAKLFASTQKSLSLIGLDNDA 239
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  270 QQLVLQLVAGILHLGNISFCE-DGNYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNVEQAAY 348
Cdd:cd14904    240 QRTLFKILSGVLHLGEVMFDKsDENGSRISNGSQLSQVAKMLGLPTTRIEEALCNRSVVT----RNESVTVPLAPVEAEE 315
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  349 TRDALAKGLYARLFDFLVEAINRAMQKPQEEYS--IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEY 426
Cdd:cd14904    316 NRDALAKAIYSKLFDWMVVKINAAISTDDDRIKgqIGVLDIFGFEDFAHNGFEQFCINYANEKLQQKFTTDVFKTVEEEY 395
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  427 VQEGIRWTPIQYFNNKVVCDLIENKLsppGIMSVLDDVCATMHatggGADQTLLQKLQAAV-----GTHEHF-NSWSAGF 500
Cdd:cd14904    396 IREGLQWDHIEYQDNQGIVEVIDGKM---GIIALMNDHLRQPR----GTEEALVNKIRTNHqtkkdNESIDFpKVKRTQF 468
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  501 VIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLF-----PEKLDGDKKGR----PSTAGSKIKKQANDLV 571
Cdd:cd14904    469 IINHYAGPVTYETVGFMEKHRDTLQNDLLDLVLLSSLDLLTELFgsseaPSETKEGKSGKgtkaPKSLGSQFKTSLSQLM 548
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  572 ATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWprWRGDERQ 651
Cdd:cd14904    549 DNIKTTNTHYVRCIKPNANKSPTEFDKRMVVEQLRSAGVIEAIRITRSGYPSRLTPKELATRYAIMFPPSM--HSKDVRR 626
                          650       660
                   ....*....|....*....|....*..
gi 1622892340  652 GVQHLLRAVNME-PDQYQMGSTKVFVK 677
Cdd:cd14904    627 TCSVFMTAIGRKsPLEYQIGKSLIYFK 653
MYSc_Myo28 cd14889
class XXVIII myosin, motor domain; These myosins are found in fish, chicken, and mollusks. The ...
37-677 2.42e-156

class XXVIII myosin, motor domain; These myosins are found in fish, chicken, and mollusks. The tail regions of these class-XXVIII myosins consist of an IQ motif, a short coiled-coil region, and an SH2 domain. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276854  Cd Length: 659  Bit Score: 480.56  E-value: 2.42e-156
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   37 LRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNML----IDCENQCVIISGES 112
Cdd:cd14889      7 LKVRFMQSNIYTYVGDILVAINPFKYLHIYEKEVSQKYKCEKKSSLPPHIFAVADRAYQSMLgrlaRGPKNQCIVISGES 86
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  113 GAGKTVAAKYIMGYISKVSGGGNKVQHVkdiILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFsRGGEPDGGKISNFLL 192
Cdd:cd14889     87 GAGKTESTKLLLRQIMELCRGNSQLEQQ---ILQVNPLLEAFGNAQTVMNDNSSRFGKYIQLRF-RNGHVKGAKINEYLL 162
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  193 EKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLN----QSDTYQVDGTDdrsdFGETLSAMQVIGIPPS 268
Cdd:cd14889    163 EKSRVVHQDGGEENFHIFYYMFAGISAEDRENYGLLDPGKYRYLNngagCKREVQYWKKK----YDEVCNAMDMVGFTEQ 238
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  269 IQQLVLQLVAGILHLGNISF-CEDGNYARVE--SVDLLAFPAYLLGIDSGRLQEKLTSRKMDSRwggrSESIDVTLNVEQ 345
Cdd:cd14889    239 EEVDMFTILAGILSLGNITFeMDDDEALKVEndSNGWLKAAAGQFGVSEEDLLKTLTCTVTFTR----GEQIQRHHTKQQ 314
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  346 AAYTRDALAKGLYARLFDFLVEAINRAMqKPQEEYS-----IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLK 420
Cdd:cd14889    315 AEDARDSIAKVAYGRVFGWIVSKINQLL-APKDDSSvelreIGILDIFGFENFAVNRFEQACINLANEQLQYFFNHHIFL 393
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  421 AEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFN---SWS 497
Cdd:cd14889    394 MEQKEYKKEGIDWKEITYKDNKPILDLFLNK--PIGILSLLDEQSHFPQAT----DESFVDKLNIHFKGNSYYGksrSKS 467
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  498 AGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLF-----------------PEKLDGDKKGRPSTAG 560
Cdd:cd14889    468 PKFTVNHYAGKVTYNASGFLEKNRDTIPASIRTLFINSATPLLSVLFtatrsrtgtlmpraklpQAGSDNFNSTRKQSVG 547
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  561 SKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPE 640
Cdd:cd14889    548 AQFKHSLGVLMEKMFAASPHFVRCIKPNHVKVPGQLDSKYIQDQLRYNGLLETIRIRREGFSWRPSFAEFAERYKILLCE 627
                          650       660       670
                   ....*....|....*....|....*....|....*..
gi 1622892340  641 twPRWRGDeRQGVQHLLRAVNMEpdQYQMGSTKVFVK 677
Cdd:cd14889    628 --PALPGT-KQSCLRILKATKLV--GWKCGKTRLFFK 659
PTZ00014 PTZ00014
myosin-A; Provisional
19-715 1.40e-155

myosin-A; Provisional


Pssm-ID: 240229 [Multi-domain]  Cd Length: 821  Bit Score: 484.15  E-value: 1.40e-155
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   19 VDDMVLLPQITEDAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYEN-PPHIYALTDNMYRNM 97
Cdd:PTZ00014    98 YGDIGLLPHTNIPCVLDFLKHRYLKNQIYTTADPLLVAINPFKDLGNTTNDWIRRYRDAKDSDKlPPHVFTTARRALENL 177
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   98 LIDCENQCVIISGESGAGKTVAAKYIMGYISKvSGGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFS 177
Cdd:PTZ00014   178 HGVKKSQTIIVSGESGAGKTEATKQIMRYFAS-SKSGNMDLKIQNAIMAANPVLEAFGNAKTIRNNNSSRFGRFMQLQLG 256
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  178 RGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNqSDTYQVDGTDDRSDFGETL 257
Cdd:PTZ00014   257 EEGGIRYGSIVAFLLEKSRVVTQEDDERSYHIFYQLLKGANDEMKEKYKLKSLEEYKYIN-PKCLDVPGIDDVKDFEEVM 335
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  258 SAMQVIGIPPSIQQLVLQLVAGILHLGNISFCE-------DGNYARVESVDLLAFPAYLLGIDSGRLQEKLTsrkMDSRW 330
Cdd:PTZ00014   336 ESFDSMGLSESQIEDIFSILSGVLLLGNVEIEGkeeggltDAAAISDESLEVFNEACELLFLDYESLKKELT---VKVTY 412
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  331 GGRSEsIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQE-EYSIGVLDIYGFEIFQKNGFEQFCINFVNEK 409
Cdd:PTZ00014   413 AGNQK-IEGPWSKDESEMLKDSLSKAVYEKLFLWIIRNLNATIEPPGGfKVFIGMLDIFGFEVFKNNSLEQLFINITNEM 491
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  410 LQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKLSppGIMSVLDDVCATMhatgGGADQTLLQKLQAAVGT 489
Cdd:PTZ00014   492 LQKNFVDIVFERESKLYKDEGISTEELEYTSNESVIDLLCGKGK--SVLSILEDQCLAP----GGTDEKFVSSCNTNLKN 565
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  490 HEHF----NSWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP--EKLDGdKKGRPSTAGSKI 563
Cdd:PTZ00014   566 NPKYkpakVDSNKNFVIKHTIGDIQYCASGFLFKNKDVLRPELVEVVKASPNPLVRDLFEgvEVEKG-KLAKGQLIGSQF 644
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  564 KKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWP 643
Cdd:PTZ00014   645 LNQLDSLMSLINSTEPHFIRCIKPNENKKPLDWNSSKVLIQLHSLSILEALQLRQLGFSYRRTFAEFLSQFKYLDLAVSN 724
                          650       660       670       680       690       700       710
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....
gi 1622892340  644 RWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVKNPESLFLLEEVRER--KFDGFARTIQKAWRRHVAVRKYEE 715
Cdd:PTZ00014   725 DSSLDPKEKAEKLLERSGLPKDSYAIGKTMVFLKKDAAKELTQIQREKlaAWEPLVSVLEALILKIKKKRKVRK 798
MYSc_Myo14 cd14876
class XIV myosin, motor domain; These myosins localize to plasma membranes of the ...
37-677 6.06e-152

class XIV myosin, motor domain; These myosins localize to plasma membranes of the intracellular parasites and may be involved in the cell invasion process. Their known functions include: transporting phagosomes to the nucleus and perturbing the developmentally regulated elimination of the macronucleus during conjugation. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. C-terminal to their motor domain these myosins have a MyTH4-FERM protein domain combination. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276843  Cd Length: 649  Bit Score: 468.70  E-value: 6.06e-152
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   37 LRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYEN-PPHIY-----ALtDNMYR-NmlidcENQCVIIS 109
Cdd:cd14876      7 LKHRYLKNQIYTTADPLLVAINPFKDLGNATDEWIRKYRDAPDLTKlPPHVFytarrAL-ENLHGvN-----KSQTIIVS 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  110 GESGAGKTVAAKYIMGYISkVSGGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISN 189
Cdd:cd14876     81 GESGAGKTEATKQIMRYFA-SAKSGNMDLRIQTAIMAANPVLEAFGNAKTIRNNNSSRFGRFMQLDVASEGGIRYGSVVA 159
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  190 FLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSdTYQVDGTDDRSDFGETLSAMQVIGIPPSI 269
Cdd:cd14876    160 FLLEKSRIVTQDDNERSYHIFYQLLKGADSEMKSKYHLLGLKEYKFLNPK-CLDVPGIDDVADFEEVLESLKSMGLTEEQ 238
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  270 QQLVLQLVAGILHLGNISFC---EDG--NYARVESVDLLAF--PAYLLGIDSGRLQEKLTSR-------KMDSRWggrse 335
Cdd:cd14876    239 IDTVFSIVSGVLLLGNVKITgktEQGvdDAAAISNESLEVFkeACSLLFLDPEALKRELTVKvtkaggqEIEGRW----- 313
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  336 sidvtlNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQ--EEYsIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQI 413
Cdd:cd14876    314 ------TKDDAEMLKLSLAKAMYDKLFLWIIRNLNSTIEPPGgfKNF-MGMLDIFGFEVFKNNSLEQLFINITNEMLQKN 386
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  414 FIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKLSppGIMSVLDDVCATMhatgGGADQTLLQKLQAAVGTHEHF 493
Cdd:cd14876    387 FIDIVFERESKLYKDEGIPTAELEYTSNAEVIDVLCGKGK--SVLSILEDQCLAP----GGSDEKFVSACVSKLKSNGKF 460
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  494 ----NSWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP-EKLDGDKKGRPSTAGSKIKKQAN 568
Cdd:cd14876    461 kpakVDSNINFIVVHTIGDIQYNAEGFLFKNKDVLRAELVEVVQASTNPVVKALFEgVVVEKGKIAKGSLIGSQFLKQLE 540
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  569 DLVaTLMRCT-PHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWRG 647
Cdd:cd14876    541 SLM-GLINSTePHFIRCIKPNETKKPLEWNSSKVLIQLHALSILEALQLRQLGYSYRRPFEEFLYQFKFLDLGIANDKSL 619
                          650       660       670
                   ....*....|....*....|....*....|
gi 1622892340  648 DERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14876    620 DPKVAALKLLESSGLSEDEYAIGKTMVFLK 649
MYSc_Myh7b cd14927
class II myosin heavy chain 7b, motor domain; Myosin motor domain of cardiac muscle, beta ...
36-677 7.17e-146

class II myosin heavy chain 7b, motor domain; Myosin motor domain of cardiac muscle, beta myosin heavy chain 7b (also called KIAA1512, dJ756N5.1, MYH14, MHC14). MYH7B is a slow-twitch myosin. Mutations in this gene result in one form of autosomal dominant hearing impairment. Multiple transcript variants encoding different isoforms have been found for this gene. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276953 [Multi-domain]  Cd Length: 676  Bit Score: 454.03  E-value: 7.17e-146
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGAG 115
Cdd:cd14927      6 NLRRRYSRWMIYTYSGLFCVTVNPYKWLPVYTAPVVAAYKGKRRSEAPPHIYAIADNAYNDMLRNRENQSMLITGESGAG 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  116 KTVAAKYIMGYISKVSGGGNKVQH------------VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPD 183
Cdd:cd14927     86 KTVNTKRVIQYFAIVAALGDGPGKkaqflatktggtLEDQIIEANPAMEAFGNAKTLRNDNSSRFGKFIRIHFGPTGKLA 165
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  184 GGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVI 263
Cdd:cd14927    166 SADIDIYLLEKSRVIFQQPGERSYHIYYQILSGKKPELQDMLLVSMNPYDYHFCSQGVTTVDNMDDGEELMATDHAMDIL 245
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  264 GIPPSIQQLVLQLVAGILHLGNISFC-----EDGNYARVESVDLlafPAYLLGIDSGRLQEKLtsrkMDSRWGGRSESID 338
Cdd:cd14927    246 GFSPDEKYGCYKIVGAIMHFGNMKFKqkqreEQAEADGTESADK---AAYLMGVSSADLLKGL----LHPRVKVGNEYVT 318
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  339 VTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAM-QKPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIEL 417
Cdd:cd14927    319 KGQSVEQVVYAVGALAKATYDRMFKWLVSRINQTLdTKLPRQFFIGVLDIAGFEIFEFNSFEQLCINFTNEKLQQFFNHH 398
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  418 TLKAEQEEYVQEGIRWTPIQYFNNKVVC-DLIENklsPPGIMSVLDDVCATMHATgggaDQTLLQKL-QAAVGTHEHFN- 494
Cdd:cd14927    399 MFILEQEEYKREGIEWVFIDFGLDLQACiDLIEK---PLGILSILEEECMFPKAS----DASFKAKLyDNHLGKSPNFQk 471
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  495 -------SWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKKGRPSTAGSKIKKQA 567
Cdd:cd14927    472 prpdkkrKYEAHFEVVHYAGVVPYNIVGWLDKNKDPLNETVVAIFQKSQNKLLATLYENYVGSDSTEDPKSGVKEKRKKA 551
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  568 --------------NDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQR 633
Cdd:cd14927    552 asfqtvsqlhkenlNKLMTNLRATQPHFVRCIIPNETKTPGVMDPFLVLHQLRCNGVLEGIRICRKGFPNRILYADFKQR 631
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|....*
gi 1622892340  634 YAILTPETWPRWR-GDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14927    632 YRILNPSAIPDDKfVDSRKATEKLLGSLDIDHTQYQFGHTKVFFK 676
MYSc_Myo30 cd14891
class XXX myosin, motor domain; Myosins of class XXX are composed of an amino-terminal ...
32-677 4.85e-145

class XXX myosin, motor domain; Myosins of class XXX are composed of an amino-terminal SH3-like domain, two IQ motifs, a coiled-coil region and a PX domain. The myosin classes XXX to XXXIV contain members from Phytophthora species and Hyaloperonospora parasitica. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276856  Cd Length: 645  Bit Score: 450.65  E-value: 4.85e-145
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYI--FTYIGSVLISVNPFKQMPyftDREIDLYQGAAQYENPPHIYALTDNMYRNMLI----DCeNQC 105
Cdd:cd14891      2 GILHNLEERSKLDNQrpYTFMANVLIAVNPLRRLP---EPDKSDYINTPLDPCPPHPYAIAEMAYQQMCLgsgrMQ-NQS 77
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  106 VIISGESGAGKTVAAKYIMGYISKVSGGGNK----------------VQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFG 169
Cdd:cd14891     78 IVISGESGAGKTETSKIILRFLTTRAVGGKKasgqdieqsskkrklsVTSLDERLMDTNPILESFGNAKTLRNHNSSRFG 157
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  170 KYFEIQFSRGG-EPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTD 248
Cdd:cd14891    158 KFMKLQFTKDKfKLAGAFIETYLLEKSRLVAQPPGERNFHIFYQLLAGASAELLKELLLLSPEDFIYLNQSGCVSDDNID 237
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  249 DRSDFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISFCE------DGNYARVESVDLLAFPAYLLGIDSGRLQEKLT 322
Cdd:cd14891    238 DAANFDNVVSALDTVGIDEDLQLQIWRILAGLLHLGNIEFDEedtsegEAEIASESDKEALATAAELLGVDEEALEKVIT 317
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  323 SRKMDSRWGGRSesidVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAM-QKPQEEYSIGVLDIYGFEIFQ-KNGFEQ 400
Cdd:cd14891    318 QREIVTRGETFT----IKRNAREAVYSRDAIAKSIYERLFLWIVQQINTSLgHDPDPLPYIGVLDIFGFESFEtKNDFEQ 393
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  401 FCINFVNEKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggaDQTLL 480
Cdd:cd14891    394 LLINYANEALQATFNQQVFIAEQELYKSEGIDVGVITWPDNRECLDLIASK--PNGILPLLDNEARNPNPS----DAKLN 467
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  481 QKLQAAVGTHEHFNSWSAG-----FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSeQAFLrmlfpekldgdkkgr 555
Cdd:cd14891    468 ETLHKTHKRHPCFPRPHPKdmremFIVKHYAGTVSYTIGSFIDKNNDIIPEDFEDLLASS-AKFS--------------- 531
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  556 pstagskikKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYA 635
Cdd:cd14891    532 ---------DQMQELVDTLEATRCNFIRCIKPNAAMKVGVFDNRYVVDQLRCSGILQTCEVLKVGLPTRVTYAELVDVYK 602
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|...
gi 1622892340  636 -ILTPETWPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14891    603 pVLPPSVTRLFAENDRTLTQAILWAFRVPSDAYRLGRTRVFFR 645
MYSc_Myh2_insects_mollusks cd14911
class II myosin heavy chain 2, motor domain; Myosin motor domain of type IIa skeletal muscle ...
36-677 6.46e-144

class II myosin heavy chain 2, motor domain; Myosin motor domain of type IIa skeletal muscle myosin heavy chain 2 (also called MYH2A, MYHSA2, MyHC-IIa, MYHas8, MyHC-2A) in insects and mollusks. This gene encodes a member of the class II or conventional myosin heavy chains, and functions in skeletal muscle contraction. Mutations in this gene results in inclusion body myopathy-3 and familial congenital myopathy. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276876 [Multi-domain]  Cd Length: 674  Bit Score: 448.66  E-value: 6.46e-144
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGAG 115
Cdd:cd14911      6 NIKDRYYSGLIYTYSGLFCVVVNPYKKLPIYTEKIMERYKGIKRHEVPPHVFAITDSAYRNMLGDREDQSILCTGESGAG 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  116 KTVAAKYIMGYI-----SKVSGGGNKVQHVKDI----------ILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGG 180
Cdd:cd14911     86 KTENTKKVIQFLayvaaSKPKGSGAVPHPAVNPavligeleqqLLQANPILEAFGNAKTVKNDNSSRFGKFIRINFDASG 165
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  181 EPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNqSDTYQVDGTDDRSDFGETLSAM 260
Cdd:cd14911    166 FISGANIETYLLEKSRAIRQAKDERTFHIFYQLLAGATPEQREKFILDDVKSYAFLS-NGSLPVPGVDDYAEFQATVKSM 244
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  261 QVIGIPPSIQQLVLQLVAGILHLGNISFCEDGNYARVESVD--LLAFPAYLLGIDSGRLQEKLTSRKMDSrwgGRsESID 338
Cdd:cd14911    245 NIMGMTSEDFNSIFRIVSAVLLFGSMKFRQERNNDQATLPDntVAQKIAHLLGLSVTDMTRAFLTPRIKV---GR-DFVT 320
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  339 VTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQ--KPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIE 416
Cdd:cd14911    321 KAQTKEQVEFAVEAIAKACYERMFKWLVNRINRSLDrtKRQGASFIGILDMAGFEIFELNSFEQLCINYTNEKLQQLFNH 400
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  417 LTLKAEQEEYVQEGIRWTPIQY-FNNKVVCDLIENklsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNS 495
Cdd:cd14911    401 TMFILEQEEYQREGIEWKFIDFgLDLQPTIDLIDK---PGGIMALLDEECWFPKAT----DKTFVDKLVSAHSMHPKFMK 473
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  496 WS----AGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFL---------------RMLFPEKLDGDKKGRP 556
Cdd:cd14911    474 TDfrgvADFAIVHYAGRVDYSAAKWLMKNMDPLNENIVSLLQGSQDPFVvniwkdaeivgmaqqALTDTQFGARTRKGMF 553
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  557 STAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAI 636
Cdd:cd14911    554 RTVSHLYKEQLAKLMDTLRNTNPNFVRCIIPNHEKRAGKIDAPLVLDQLRCNGVLEGIRICRQGFPNRIPFQEFRQRYEL 633
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|.
gi 1622892340  637 LTPETWPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14911    634 LTPNVIPKGFMDGKKACEKMIQALELDSNLYRVGQSKIFFR 674
MYSc_Myo47 cd14908
class XLVII myosin, motor domain; The class XLVII myosins are comprised of Stramenopiles. Not ...
32-677 1.59e-143

class XLVII myosin, motor domain; The class XLVII myosins are comprised of Stramenopiles. Not much is known about this myosin class. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276873 [Multi-domain]  Cd Length: 682  Bit Score: 447.82  E-value: 1.59e-143
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTdREI------DLYQGAAQYENP----PHIYALTDNMYRNMLIDC 101
Cdd:cd14908      2 AILHSLSRRFFRGIIYTWTGPVLIAVNPFQRLPLYG-KEIlesyrqEGLLRSQGIESPqalgPHVFAIADRSYRQMMSEI 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  102 E-NQCVIISGESGAGKTVAAKYIMGYISKVSGGGNKVQH---------VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKY 171
Cdd:cd14908     81 RaSQSILISGESGAGKTESTKIVMLYLTTLGNGEEGAPNegeelgklsIMDRVLQSNPILEAFGNARTLRNDNSSRFGKF 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  172 FEIQFSRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQ--------NLGLMTPDYYYYLNQSDTYQ 243
Cdd:cd14908    161 IELGFNRAGNLLGAKVQTYLLEKVRLPFHASGERNYHIFYQLLRGGDEEEHEkyefhdgiTGGLQLPNEFHYTGQGGAPD 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  244 VDGTDDRSDFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISF---CEDG--NYARVESVDLLAFPAYLLGIDSGRLQ 318
Cdd:cd14908    241 LREFTDEDGLVYTLKAMRTMGWEESSIDTILDIIAGLLHLGQLEFeskEEDGaaEIAEEGNEKCLARVAKLLGVDVDKLL 320
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  319 EKLTSRKMDSrwggRSESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAM---QKPQEEYSIGVLDIYGFEIFQK 395
Cdd:cd14908    321 RALTSKIIVV----RGKEITTKLTPHKAYDARDALAKTIYGALFLWVVATVNSSInweNDKDIRSSVGVLDIFGFECFAH 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  396 NGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCaTMHATGGGA 475
Cdd:cd14908    397 NSFEQLCINFTNEALQQQFNQFIFKLEQKEYEKESIEWAFIEFPDNQDCLDTIQAK--KKGILTMLDDEC-RLGIRGSDA 473
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  476 D------QTLLQKLQAAVGTHEHFNSWSAG-----FVIHHYAGKVSYDV-SGFCERNRDvlfsdliELMQTSEQAFlrml 543
Cdd:cd14908    474 NyasrlyETYLPEKNQTHSENTRFEATSIQktkliFAVRHFAGQVQYTVeTTFCEKNKD-------EIPLTADSLF---- 542
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  544 fpekldgdkkgrpsTAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAY 623
Cdd:cd14908    543 --------------ESGQQFKAQLHSLIEMIEDTDPHYIRCIKPNDAAKPDLVTRKRVTEQLRYGGVLEAVRVARSGYPV 608
                          650       660       670       680       690       700       710
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....
gi 1622892340  624 RRQFAKFLQRYAIL---TPETWPRWRGDERQG-----------------VQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14908    609 RLPHKDFFKRYRMLlplIPEVVLSWSMERLDPqklcvkkmckdlvkgvlSPAMVSMKNIPEDTMQLGKSKVFMR 682
MYSc_Myh18 cd14932
class II myosin heavy chain 18, motor domain; Myosin motor domain of muscle myosin heavy chain ...
32-677 1.59e-142

class II myosin heavy chain 18, motor domain; Myosin motor domain of muscle myosin heavy chain 18. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276895 [Multi-domain]  Cd Length: 676  Bit Score: 445.24  E-value: 1.59e-142
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14932      2 SVLHNLKERYYSGLIYTYSGLFCVVINPYKYLPIYSEEIVNMYKGKKRHEMPPHIYAITDTAYRSMMQDREDQSILCTGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSG--------GGNKVQH--VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGE 181
Cdd:cd14932     82 SGAGKTENTKKVIQYLAYVASsfktkkdqSSIALSHgeLEKQLLQANPILEAFGNAKTVKNDNSSRFGKFIRINFDVNGY 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  182 PDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTyQVDGTDDRSDFGETLSAMQ 261
Cdd:cd14932    162 IVGANIETYLLEKSRAIRQAKDERAFHIFYYLLTGAGDKLRSELCLEDYSKYRFLSNGNV-TIPGQQDKELFAETMEAFR 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  262 VIGIPPSIQQLVLQLVAGILHLGNISFCEDGNYARVESVDLLAFP--AYLLGIDSGRLQEKLTSRKMDSrwgGRsESIDV 339
Cdd:cd14932    241 IMSIPEEEQTGLLKVVSAVLQLGNMSFKKERNSDQASMPDDTAAQkvCHLLGMNVTDFTRAILSPRIKV---GR-DYVQK 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  340 TLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS--IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIEL 417
Cdd:cd14932    317 AQTQEQAEFAVEALAKASYERMFRWLVMRINKALDKTKRQGAsfIGILDIAGFEIFELNSFEQLCINYTNEKLQQLFNHT 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  418 TLKAEQEEYVQEGIRWTPIQYFNNKVVC-DLIENKLSPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNSW 496
Cdd:cd14932    397 MFILEQEEYQREGIEWSFIDFGLDLQPCiELIEKPNGPPGILALLDEECWFPKAT----DKSFVEKVVQEQGNNPKFQKP 472
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  497 S-----AGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFL--------RMLFPEKLDG----------DKK 553
Cdd:cd14932    473 KklkddADFCIIHYAGKVDYKANEWLMKNMDPLNENVATLLNQSTDKFVselwkdvdRIVGLDKVAGmgeslhgafkTRK 552
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  554 GRPSTAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQR 633
Cdd:cd14932    553 GMFRTVGQLYKEQLMNLMTTLRNTNPNFVRCIIPNHEKKAGKLAHHLVLDQLRCNGVLEGIRICRQGFPNRIVFQEFRQR 632
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|....
gi 1622892340  634 YAILTPETWPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14932    633 YEILTPNAIPKGFMDGKQACVLMVKALELDPNLYRIGQSKVFFR 676
MYSc_Myh16 cd14934
class II myosin heavy chain 16, motor domain; Myosin motor domain of myosin heavy chain 16 ...
32-677 6.28e-142

class II myosin heavy chain 16, motor domain; Myosin motor domain of myosin heavy chain 16 pseudogene (also called MHC20, MYH16, and myh5), encoding a sarcomeric myosin heavy chain expressed in nonhuman primate masticatory muscles, is inactivated in humans. This cd contains Myh16 in mammals. MYH16 has intermediate fibres between that of slow type 1 and fast 2B fibres, but exert more force than any other fibre type examined. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. Some of the data used for this classification were produced by the CyMoBase team at the Max-Planck-Institute for Biophysical Chemistry. The sequence names are composed of the species abbreviation followed by the protein abbreviation and optional protein classifier and variant designations.


Pssm-ID: 276896 [Multi-domain]  Cd Length: 659  Bit Score: 442.93  E-value: 6.28e-142
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14934      2 SVLDNLRQRYTNMRIYTYSGLFCVTVNPYKWLPIYGARVANMYKGKKRTEMPPHLFSISDNAYHDMLMDRENQSMLITGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVQ----HVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKI 187
Cdd:cd14934     82 SGAGKTENTKKVIQYFANIGGTGKQSSdgkgSLEDQIIQANPVLEAFGNAKTTRNNNSSRFGKFIRIHFGTTGKLAGADI 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  188 SNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLM-TPDYYYYLNQSDTYqVDGTDDRSDFGETLSAMQVIGIP 266
Cdd:cd14934    162 ESYLLEKSRVISQQAAERGYHIFYQILSNKKPELIESLLLVpNPKEYHWVSQGVTV-VDNMDDGEELQITDVAFDVLGFS 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  267 PSIQQLVLQLVAGILHLGNISFCEDG--NYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNVE 344
Cdd:cd14934    241 AEEKIGVYKLTGGIMHFGNMKFKQKPreEQAEVDTTEVADKVAHLMGLNSGELQKGITRPRVKV----GNEFVQKGQNME 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  345 QAAYTRDALAKGLYARLFDFLVEAINRAMQ-KPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQ 423
Cdd:cd14934    317 QCNNSIGALGKAVYDKMFKWLVVRINKTLDtKMQRQFFIGVLDIAGFEIFEFNSFEQLCINFTNEKLQQFFNHHMFVLEQ 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  424 EEYVQEGIRWTPIQYFNNKVVC-DLIENklsPPGIMSVLDDVCATMHATgggaDQTLLQKL-QAAVGTHEHFNSWSAG-- 499
Cdd:cd14934    397 EEYKREGIEWVFIDFGLDLQACiDLLEK---PMGIFSILEEQCVFPKAT----DATFKAALyDNHLGKSSNFLKPKGGkg 469
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  500 ------FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEK--LDGDKKGRPS----TAGSKIKKQA 567
Cdd:cd14934    470 kgpeahFELVHYAGTVGYNITGWLEKNKDPLNETVVGLFQKSSLGLLALLFKEEeaPAGSKKQKRGssfmTVSNFYREQL 549
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  568 NDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWRG 647
Cdd:cd14934    550 NKLMTTLHSTAPHFVRCIVPNEFKQSGVVDAHLIMHQLACNGVLEGIRICRKGFPNRLQYPEFKQRYQVLNPNVIPQGFV 629
                          650       660       670
                   ....*....|....*....|....*....|
gi 1622892340  648 DERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14934    630 DNKKASELLLGSIDLDVNEYKIGHTKVFFR 659
MYSc_Myh15_mammals cd14929
class II myosin heavy chain 15, motor domain; Myosin motor domain of sarcomeric myosin heavy ...
37-677 2.21e-140

class II myosin heavy chain 15, motor domain; Myosin motor domain of sarcomeric myosin heavy chain 15 in mammals (also called KIAA1000) . MYH15 is a slow-twitch myosin. Myh15 is a ventricular myosin heavy chain. Myh15 is absent in embryonic and fetal muscles and is found in orbital layer of extraocular muscles at birth. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276892 [Multi-domain]  Cd Length: 662  Bit Score: 439.03  E-value: 2.21e-140
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   37 LRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGAGK 116
Cdd:cd14929      7 LRRRYDHWMIYTYSGLFCVTINPYKWLPVYQKEVMAAYKGKRRSEAPPHIFAVANNAFQDMLHNRENQSILFTGESGAGK 86
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  117 TVAAKYIMGYISKVSGGG---NKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNFLLE 193
Cdd:cd14929     87 TVNTKHIIQYFATIAAMIeskKKLGALEDQIMQANPVLEAFGNAKTLRNDNSSRFGKFIRMHFGARGMLSSADIDIYLLE 166
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  194 KSRVVMQNENERNFHIYYQLLEGaSQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSIQQLV 273
Cdd:cd14929    167 KSRVIFQQPGERNYHIFYQILSG-KKELRDLLLVSANPSDFHFCSCGAVAVESLDDAEELLATEQAMDILGFLPDEKYGC 245
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  274 LQLVAGILHLGNISFCEDGNYARVES--VDLLAFPAYLLGIDSGRLQEKLTSR--KMDSRWGGRSEsidvtlNVEQAAYT 349
Cdd:cd14929    246 YKLTGAIMHFGNMKFKQKPREEQLEAdgTENADKAAFLMGINSSELVKGLIHPriKVGNEYVTRSQ------NIEQVTYA 319
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  350 RDALAKGLYARLFDFLVEAINRAMQ-KPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQ 428
Cdd:cd14929    320 VGALSKSIYERMFKWLVARINRVLDaKLSRQFFIGILDITGFEILDYNSLEQLCINFTNEKLQQFFNQHMFVLEQEEYRK 399
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  429 EGIRWTPIQYFNNKVVC-DLIENklsPPGIMSVLDDVCATMHATgggaDQTLLQKL-QAAVGTHEHFN-------SWSAG 499
Cdd:cd14929    400 EGIDWVSIDFGLDLQACiDLIEK---PMGIFSILEEECMFPKAT----DLTFKTKLfDNHFGKSVHFQkpkpdkkKFEAH 472
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  500 FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLD-------GDKKGRPSTAGSKI----KKQAN 568
Cdd:cd14929    473 FELVHYAGVVPYNISGWLEKNKDLLNETVVAVFQKSSNRLLASLFENYIStdsaiqfGEKKRKKGASFQTVaslhKENLN 552
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  569 DLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWR-G 647
Cdd:cd14929    553 KLMTNLKSTAPHFVRCINPNVNKIPGVLDPYLVLQQLRCNGVLEGIRICREGFPNRLLYADFKQRYCILNPRTFPKSKfV 632
                          650       660       670
                   ....*....|....*....|....*....|
gi 1622892340  648 DERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14929    633 SSRKAAEELLGSLEIDHTQYRFGITKVFFK 662
MYSc_Myh3 cd14913
class II myosin heavy chain 3, motor domain; Myosin motor domain of fetal skeletal muscle ...
32-677 4.39e-140

class II myosin heavy chain 3, motor domain; Myosin motor domain of fetal skeletal muscle myosin heavy chain 3 (MYHC-EMB, MYHSE1, HEMHC, SMHCE) in tetrapods including mammals, lizards, and frogs. This gene is a member of the MYH family and encodes a protein with an IQ domain and a myosin head-like domain. Mutations in this gene have been associated with two congenital contracture (arthrogryposis) syndromes, Freeman-Sheldon syndrome and Sheldon-Hall syndrome. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276878 [Multi-domain]  Cd Length: 668  Bit Score: 438.33  E-value: 4.39e-140
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14913      2 AVLYNLKDRYTSWMIYTYSGLFCVTVNPYKWLPVYNPEVVEGYRGKKRQEAPPHIFSISDNAYQFMLTDRENQSILITGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVQH--------VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPD 183
Cdd:cd14913     82 SGAGKTVNTKRVIQYFATIAATGDLAKKkdskmkgtLEDQIISANPLLEAFGNAKTVRNDNSSRFGKFIRIHFGTTGKLA 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  184 GGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDY-YYYLNQSDTyQVDGTDDRSDFGETLSAMQV 262
Cdd:cd14913    162 SADIETYLLEKSRVTFQLKAERSYHIFYQILSNKKPELIELLLITTNPYdYPFISQGEI-LVASIDDAEELLATDSAIDI 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  263 IGIPPSIQQLVLQLVAGILHLGNISFCEDGNYARVE--SVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVT 340
Cdd:cd14913    241 LGFTPEEKSGLYKLTGAVMHYGNMKFKQKQREEQAEpdGTEVADKTAYLMGLNSSDLLKALCFPRVKV----GNEYVTKG 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  341 LNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQ-KPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTL 419
Cdd:cd14913    317 QTVDQVHHAVNALSKSVYEKLFLWMVTRINQQLDtKLPRQHFIGVLDIAGFEIFEYNSLEQLCINFTNEKLQQFFNHHMF 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  420 KAEQEEYVQEGIRWTPIQYFNNKVVC-DLIENklsPPGIMSVLDDVCATMHATGGG-----ADQTL-----LQKLQAAVG 488
Cdd:cd14913    397 VLEQEEYKKEGIEWTFIDFGMDLAACiELIEK---PMGIFSILEEECMFPKATDTSfknklYDQHLgksnnFQKPKVVKG 473
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  489 THEhfnswsAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP--EKLDGD--------KKGRP-S 557
Cdd:cd14913    474 RAE------AHFSLIHYAGTVDYSVSGWLEKNKDPLNETVVGLYQKSSNRLLAHLYAtfATADADsgkkkvakKKGSSfQ 547
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  558 TAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAIL 637
Cdd:cd14913    548 TVSALFRENLNKLMSNLRTTHPHFVRCIIPNETKTPGAMEHSLVLHQLRCNGVLEGIRICRKGFPNRILYGDFKQRYRVL 627
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|.
gi 1622892340  638 TPETWPRWRG-DERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14913    628 NASAIPEGQFiDSKKACEKLLASIDIDHTQYKFGHTKVFFK 668
MYSc_Myh1_insects_crustaceans cd14909
class II myosin heavy chain 1, motor domain; Myosin motor domain of type IIx skeletal muscle ...
32-677 3.19e-139

class II myosin heavy chain 1, motor domain; Myosin motor domain of type IIx skeletal muscle myosin heavy chain 1 (also called MYHSA1, MYHa, MyHC-2X/D, MGC133384) in insects and crustaceans. Myh1 is a type I skeletal muscle myosin that in Humans is encoded by the MYH1 gene. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276874  Cd Length: 666  Bit Score: 436.19  E-value: 3.19e-139
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14909      2 SVLHNLRQRYYAKLIYTYSGLFCVAINPYKRYPVYTNRCAKMYRGKRRNEVPPHIFAISDGAYVDMLTNHVNQSMLITGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYI------SKVSGGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGG 185
Cdd:cd14909     82 SGAGKTENTKKVIAYFatvgasKKTDEAAKSKGSLEDQVVQTNPVLEAFGNAKTVRNDNSSRFGKFIRIHFGPTGKLAGA 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  186 KISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDY-YYYLNQSDTyQVDGTDDRSDFGETLSAMQVIG 264
Cdd:cd14909    162 DIETYLLEKARVISQQSLERSYHIFYQIMSGSVPGVKEMCLLSDNIYdYYIVSQGKV-TVPNVDDGEEFSLTDQAFDILG 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  265 IPPSIQQLVLQLVAGILHLGNISFCEDGNYARVES--VDLLAFPAYLLGIDSGRLQEKLtsrkMDSRWGGRSESIDVTLN 342
Cdd:cd14909    241 FTKQEKEDVYRITAAVMHMGGMKFKQRGREEQAEQdgEEEGGRVSKLFGCDTAELYKNL----LKPRIKVGNEFVTQGRN 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  343 VEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQE-EYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKA 421
Cdd:cd14909    317 VQQVTNSIGALCKGVFDRLFKWLVKKCNETLDTQQKrQHFIGVLDIAGFEIFEYNGFEQLCINFTNEKLQQFFNHHMFVL 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  422 EQEEYVQEGIRWTPIQYFNNKVVC-DLIENklsPPGIMSVLDDVCATMHATgggaDQTLLQKLQAA-VGTHEHF------ 493
Cdd:cd14909    397 EQEEYKREGIDWAFIDFGMDLLACiDLIEK---PMGILSILEEESMFPKAT----DQTFSEKLTNThLGKSAPFqkpkpp 469
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  494 --NSWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEK------LDGDKKGRP------STA 559
Cdd:cd14909    470 kpGQQAAHFAIAHYAGCVSYNITGWLEKNKDPLNDTVVDQFKKSQNKLLIEIFADHagqsggGEQAKGGRGkkgggfATV 549
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  560 GSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTP 639
Cdd:cd14909    550 SSAYKEQLNSLMTTLRSTQPHFVRCIIPNEMKQPGVVDAHLVMHQLTCNGVLEGIRICRKGFPNRMMYPDFKMRYKILNP 629
                          650       660       670
                   ....*....|....*....|....*....|....*...
gi 1622892340  640 ETwPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14909    630 AG-IQGEEDPKKAAEIILESIALDPDQYRLGHTKVFFR 666
MYSc_Myo34 cd14895
class XXXIV myosin, motor domain; Class XXXIV myosins are composed of an IQ motif, a short ...
37-677 2.93e-138

class XXXIV myosin, motor domain; Class XXXIV myosins are composed of an IQ motif, a short coiled-coil region, 5 tandem ANK repeats, and a carboxy-terminal FYVE domain. The myosin classes XXX to XXXIV contain members from Phytophthora species and Hyaloperonospora parasitica. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276860 [Multi-domain]  Cd Length: 704  Bit Score: 434.77  E-value: 2.93e-138
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   37 LRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDreIDLYQGA--AQYENPPHIYALTDNMYRNMLIDC-------ENQCVI 107
Cdd:cd14895      7 LAQRYGVDQVYCRSGAVLIAVNPFKHIPGLYD--LHKYREEmpGWTALPPHVFSIAEGAYRSLRRRLhepgaskKNQTIL 84
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  108 ISGESGAGKTVAAKYIMGYISKVS-----GGGNKVQH--VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSrGG 180
Cdd:cd14895     85 VSGESGAGKTETTKFIMNYLAESSkhttaTSSSKRRRaiSGSELLSANPILESFGNARTLRNDNSSRFGKFVRMFFE-GH 163
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  181 EPD------GGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQE--QRQNLGLMTPDYYYYLNQSDTYQV-DGTDDRS 251
Cdd:cd14895    164 ELDtslrmiGTSVETYLLEKVRVVHQNDGERNFHVFYELLAGAADDmkLELQLELLSAQEFQYISGGQCYQRnDGVRDDK 243
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  252 DFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISFC-------EDGNYARVESVDL-------------LAFPAYLLG 311
Cdd:cd14895    244 QFQLVLQSMKVLGFTDVEQAAIWKILSALLHLGNVLFVassedegEEDNGAASAPCRLasaspssltvqqhLDIVSKLFA 323
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  312 IDSGRLQEKLTSRKMDSrwGGrsESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS---------- 381
Cdd:cd14895    324 VDQDELVSALTTRKISV--GG--ETFHANLSLAQCGDARDAMARSLYAFLFQFLVSKVNSASPQRQFALNpnkaankdtt 399
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  382 --IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMS 459
Cdd:cd14895    400 pcIAVLDIFGFEEFEVNQFEQFCINYANEKLQYQFIQDILLTEQQAHIEEGIKWNAVDYEDNSVCLEMLEQR--PSGIFS 477
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  460 VLDDVCATMHATGGGADQTLLQKLQaavgTHEHFNS-----WSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQT 534
Cdd:cd14895    478 LLDEECVVPKGSDAGFARKLYQRLQ----EHSNFSAsrtdqADVAFQIHHYAGAVRYQAEGFCEKNKDQPNAELFSVLGK 553
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  535 SEQAFLRMLF--------PEKLDGDKKGRPSTA-------GSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEEN 599
Cdd:cd14895    554 TSDAHLRELFeffkasesAELSLGQPKLRRRSSvlssvgiGSQFKQQLASLLDVVQQTQTHYIRCIKPNDESASDQFDMA 633
                          650       660       670       680       690       700       710
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....
gi 1622892340  600 RVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAIL-TPETWPRWRGDErqgvqhLLRAVNMepDQYQMGSTKVFVK 677
Cdd:cd14895    634 KVSSQLRYGGVLKAVEIMRQSYPVRMKHADFVKQYRLLvAAKNASDATASA------LIETLKV--DHAELGKTRVFLR 704
MYSc_Myo39 cd14900
class XXXIX myosin, motor domain; The class XXXIX myosins are found in Stramenopiles. Not much ...
31-644 4.53e-137

class XXXIX myosin, motor domain; The class XXXIX myosins are found in Stramenopiles. Not much is known about this myosin class. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276865  Cd Length: 627  Bit Score: 428.96  E-value: 4.53e-137
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   31 DAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMP--YFTDReidLYQGAAQYEN-------------PPHIYALTDNMYR 95
Cdd:cd14900      1 TTILSALETRFYAQKIYTNTGAILLAVNPFQKLPglYSSDT---MAKYLLSFEArssstrnkgsdpmPPHIYQVAGEAYK 77
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   96 NMLI----DCENQCVIISGESGAGKTVAAKYIMGYISKV--------SGGGNKVQHVKDIILQSNPLLEAFGNAKTVRNN 163
Cdd:cd14900     78 AMMLglngVMSDQSILVSGESGSGKTESTKFLMEYLAQAgdnnlaasVSMGKSTSGIAAKVLQTNILLESFGNARTLRND 157
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  164 NSSRFGKYFEIQFSRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQnlglmtpdyyyylnqsdtyq 243
Cdd:cd14900    158 NSSRFGKFIKLHFTSGGRLTGASIQTYLLEKVRLVSQSKGERNYHIFYEMAIGASEAARK-------------------- 217
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  244 vdgtddRSDFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISFCEDGNYARV---------ESVDLLAFPAYLLGIDS 314
Cdd:cd14900    218 ------RDMYRRVMDAMDIIGFTPHERAGIFDLLAALLHIGNLTFEHDENSDRLgqlksdlapSSIWSRDAAATLLSVDA 291
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  315 GRLQEKLTSRKMdsRWGgrSESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS------IGVLDIY 388
Cdd:cd14900    292 TKLEKALSVRRI--RAG--TDFVSMKLSAAQANNARDALAKALYGRLFDWLVGKMNAFLKMDDSSKShgglhfIGILDIF 367
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  389 GFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATM 468
Cdd:cd14900    368 GFEVFPKNSFEQLCINFANETLQQQFNDYVFKAEQREYESQGVDWKYVEFCDNQDCVNLISQR--PTGILSLIDEECVMP 445
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  469 HatggGADQTLLQKLQAAVGTHEHFNSWSAG-----FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTseqaflrml 543
Cdd:cd14900    446 K----GSDTTLASKLYRACGSHPRFSASRIQrarglFTIVHYAGHVEYSTDGFLEKNKDVLHQEAVDLFVY--------- 512
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  544 fpekldgdkkgrpstaGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAY 623
Cdd:cd14900    513 ----------------GLQFKEQLTTLLETLQQTNPHYVRCLKPNDLCKAGIYERERVLNQLRCNGVMEAVRVARAGFPI 576
                          650       660
                   ....*....|....*....|.
gi 1622892340  624 RRQFAKFLQRYAILTPETWPR 644
Cdd:cd14900    577 RLLHDEFVARYFSLARAKNRL 597
MYSc_Myh9 cd14919
class II myosin heavy chain 9, motor domain; Myosin motor domain of non-muscle myosin heavy ...
32-677 7.00e-137

class II myosin heavy chain 9, motor domain; Myosin motor domain of non-muscle myosin heavy chain 9 (also called NMMHCA, NMHC-II-A, MHA, FTNS, EPSTS, and DFNA17). Myosin is a hexameric protein composed of a pair of myosin heavy chains (MYH) and two pairs of nonidentical light chains. The encoded protein is a myosin IIA heavy chain that contains an IQ domain and a myosin head-like domain which is involved in several important functions, including cytokinesis, cell motility and maintenance of cell shape. Defects in this gene have been associated with non-syndromic sensorineural deafness autosomal dominant type 17, Epstein syndrome, Alport syndrome with macrothrombocytopenia, Sebastian syndrome, Fechtner syndrome and macrothrombocytopenia with progressive sensorineural deafness. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276883 [Multi-domain]  Cd Length: 670  Bit Score: 429.90  E-value: 7.00e-137
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14919      2 SVLHNLKERYYSGLIYTYSGLFCVVINPYKNLPIYSEEIVEMYKGKKRHEMPPHIYAITDTAYRSMMQDREDQSILCTGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVQHVKDI---ILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKIS 188
Cdd:cd14919     82 SGAGKTENTKKVIQYLAHVASSHKSKKDQGELerqLLQANPILEAFGNAKTVKNDNSSRFGKFIRINFDVNGYIVGANIE 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  189 NFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTyQVDGTDDRSDFGETLSAMQVIGIPPS 268
Cdd:cd14919    162 TYLLEKSRAIRQAKEERTFHIFYYLLSGAGEHLKTDLLLEPYNKYRFLSNGHV-TIPGQQDKDMFQETMEAMRIMGIPEE 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  269 IQQLVLQLVAGILHLGNISFCEDGNYARVESVDLLAFP--AYLLGIDSGRLQEKLTSRKMDSrwgGRsESIDVTLNVEQA 346
Cdd:cd14919    241 EQMGLLRVISGVLQLGNIVFKKERNTDQASMPDNTAAQkvSHLLGINVTDFTRGILTPRIKV---GR-DYVQKAQTKEQA 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  347 AYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS--IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQE 424
Cdd:cd14919    317 DFAIEALAKATYERMFRWLVLRINKALDKTKRQGAsfIGILDIAGFEIFDLNSFEQLCINYTNEKLQQLFNHTMFILEQE 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  425 EYVQEGIRWTPIQYFNNKVVC-DLIENKLSPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNSW-----SA 498
Cdd:cd14919    397 EYQREGIEWNFIDFGLDLQPCiDLIEKPAGPPGILALLDEECWFPKAT----DKSFVEKVVQEQGTHPKFQKPkqlkdKA 472
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  499 GFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPE----------------KLDG---DKKGRPSTA 559
Cdd:cd14919    473 DFCIIHYAGKVDYKADEWLMKNMDPLNDNIATLLHQSSDKFVSELWKDvdriigldqvagmsetALPGafkTRKGMFRTV 552
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  560 GSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTP 639
Cdd:cd14919    553 GQLYKEQLAKLMATLRNTNPNFVRCIIPNHEKKAGKLDPHLVLDQLRCNGVLEGIRICRQGFPNRVVFQEFRQRYEILTP 632
                          650       660       670
                   ....*....|....*....|....*....|....*...
gi 1622892340  640 ETWPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14919    633 NSIPKGFMDGKQACVLMIKALELDSNLYRIGQSKVFFR 670
MYSc_Myo45 cd14906
class XLV myosin, motor domain; The class XLVI myosins are comprised of slime molds ...
33-637 2.21e-136

class XLV myosin, motor domain; The class XLVI myosins are comprised of slime molds Dictyostelium and Polysphondylium. Not much is known about this myosin class. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276871 [Multi-domain]  Cd Length: 715  Bit Score: 430.17  E-value: 2.21e-136
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   33 IAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIdLYQGAAQ---YENPPHIYALTDNMYRNMLIDCENQCVIIS 109
Cdd:cd14906      3 ILNNLGKRYKSDSIYTYIGNVLISINPYKDISSIYSNLI-LNEYKDInqnKSPIPHIYAVALRAYQSMVSEKKNQSIIIS 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  110 GESGAGKTVAAKYIMGYISKVSGG-----------GNKVQhvKDIiLQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQF-S 177
Cdd:cd14906     82 GESGSGKTEASKTILQYLINTSSSnqqqnnnnnnnNNSIE--KDI-LTSNPILEAFGNSRTTKNHNSSRFGKFLKIEFrS 158
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  178 RGGEPDGGKISNFLLEKSRVVMQNENER-NFHIYYQLLEGASQEQRQNLGLMT-PDYYYYLNQSDTY-------QVDGTD 248
Cdd:cd14906    159 SDGKIDGASIETYLLEKSRISHRPDNINlSYHIFYYLVYGASKDERSKWGLNNdPSKYRYLDARDDVissfksqSSNKNS 238
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  249 DRSDFGETLSAMQVI-----GIPPSIQQL--VLQLVAGILHLGNISFCEDGNYARVESV-----DLLAFPAYLLGIDSGR 316
Cdd:cd14906    239 NHNNKTESIESFQLLkqsmeSMSINKEQCdaIFLSLAAILHLGNIEFEEDSDFSKYAYQkdkvtASLESVSKLLGYIESV 318
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  317 LQEKLTSRKMDSrwGGRSESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAM-----QKPQEEYS-------IGV 384
Cdd:cd14906    319 FKQALLNRNLKA--GGRGSVYCRPMEVAQSEQTRDALSKSLYVRLFKYIVEKINRKFnqntqSNDLAGGSnkknnlfIGV 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  385 LDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDV 464
Cdd:cd14906    397 LDIFGFENLSSNSLEQLLINFTNEKLQQQFNLNVFENEQKEYLSEGIPWSNSNFIDNKECIELIEKK--SDGILSLLDDE 474
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  465 CATMHatggGADQTLLQKL-QAAVGTHEHFNSWSAG--FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLR 541
Cdd:cd14906    475 CIMPK----GSEQSLLEKYnKQYHNTNQYYQRTLAKgtLGIKHFAGDVTYQTDGWLEKNRDSLYSDVEDLLLASSNFLKK 550
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  542 MLFPEKL-----DGDKKGRPSTAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRV 616
Cdd:cd14906    551 SLFQQQItsttnTTKKQTQSNTVSGQFLEQLNQLIQTINSTSVHYIRCIKPNQTMDCNNFNNVHVLSQLRNVGVLNTIKV 630
                          650       660
                   ....*....|....*....|.
gi 1622892340  617 RRAGFAYRRQFAKFLQRYAIL 637
Cdd:cd14906    631 RKMGYSYRRDFNQFFSRYKCI 651
MYSc_Myh19 cd15896
class II myosin heavy chain19, motor domain; Myosin motor domain of muscle myosin heavy chain ...
32-677 7.72e-135

class II myosin heavy chain19, motor domain; Myosin motor domain of muscle myosin heavy chain 19. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276899 [Multi-domain]  Cd Length: 675  Bit Score: 424.86  E-value: 7.72e-135
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd15896      2 SVLHNLKERYYSGLIYTYSGLFCVVINPYKNLPIYSEEIVEMYKGKKRHEMPPHIYAITDTAYRSMMQDREDQSILCTGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGG-------GNKVQHVKDI---ILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGE 181
Cdd:cd15896     82 SGAGKTENTKKVIQYLAHVASShktkkdqNSLALSHGELekqLLQANPILEAFGNAKTVKNDNSSRFGKFIRINFDVNGY 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  182 PDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTyQVDGTDDRSDFGETLSAMQ 261
Cdd:cd15896    162 IVGANIETYLLEKSRAIRQAKEERTFHIFYYLLTGAGDKLRSELLLENYNNYRFLSNGNV-TIPGQQDKDLFTETMEAFR 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  262 VIGIPPSIQQLVLQLVAGILHLGNISFCEDGNYARVESVDLLAFP--AYLLGIDSGRLQEKLTSRKMDSrwgGRsESIDV 339
Cdd:cd15896    241 IMGIPEDEQIGMLKVVASVLQLGNMSFKKERHTDQASMPDNTAAQkvCHLMGMNVTDFTRAILSPRIKV---GR-DYVQK 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  340 TLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS--IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIEL 417
Cdd:cd15896    317 AQTQEQAEFAVEALAKATYERMFRWLVMRINKALDKTKRQGAsfIGILDIAGFEIFELNSFEQLCINYTNEKLQQLFNHT 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  418 TLKAEQEEYVQEGIRWTPIQYFNNKVVC-DLIENKLSPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNSW 496
Cdd:cd15896    397 MFILEQEEYQREGIEWSFIDFGLDLQPCiDLIEKPASPPGILALLDEECWFPKAT----DKSFVEKVLQEQGTHPKFFKP 472
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  497 -----SAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP--------EKLDG---------DKKG 554
Cdd:cd15896    473 kklkdEADFCIIHYAGKVDYKADEWLMKNMDPLNDNVATLLNQSTDKFVSELWKdvdrivglDKVSGmsempgafkTRKG 552
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  555 RPSTAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRY 634
Cdd:cd15896    553 MFRTVGQLYKEQLSKLMATLRNTNPNFVRCIIPNHEKKAGKLDPHLVLDQLRCNGVLEGIRICRQGFPNRIVFQEFRQRY 632
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|...
gi 1622892340  635 AILTPETWPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd15896    633 EILTPNAIPKGFMDGKQACVLMIKSLELDPNLYRIGQSKVFFR 675
MYSc_Myh11 cd14921
class II myosin heavy chain 11, motor domain; Myosin motor domain of smooth muscle myosin ...
32-677 4.49e-134

class II myosin heavy chain 11, motor domain; Myosin motor domain of smooth muscle myosin heavy chain 11 (also called SMMHC, SMHC). The gene product is a subunit of a hexameric protein that consists of two heavy chain subunits and two pairs of non-identical light chain subunits. It functions as a major contractile protein, converting chemical energy into mechanical energy through the hydrolysis of ATP. The gene encoding a human ortholog of rat NUDE1 is transcribed from the reverse strand of this gene, and its 3' end overlaps with that of the latter. Inversion of the MYH11 locus is one of the most frequent chromosomal aberrations found in acute myeloid leukemia. Alternative splicing generates isoforms that are differentially expressed, with ratios changing during muscle cell maturation. Mutations in MYH11 have been described in individuals with thoracic aortic aneurysms leading to acute aortic dissections with patent ductus arteriosus. MYH11 mutations are also thought to contribute to human colorectal cancer and are also associated with Peutz-Jeghers syndrome. The mutations found in human intestinal neoplasia result in unregulated proteins with constitutive motor activity, similar to the mutant myh11 zebrafish. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276885 [Multi-domain]  Cd Length: 673  Bit Score: 422.89  E-value: 4.49e-134
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14921      2 SVLHNLRERYFSGLIYTYSGLFCVVVNPYKHLPIYSEKIVDMYKGKKRHEMPPHIYAIADTAYRSMLQDREDQSILCTGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKV--SGGGNK----VQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGG 185
Cdd:cd14921     82 SGAGKTENTKKVIQYLAVVasSHKGKKdtsiTGELEKQLLQANPILEAFGNAKTVKNDNSSRFGKFIRINFDVTGYIVGA 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  186 KISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTyQVDGTDDRSDFGETLSAMQVIGI 265
Cdd:cd14921    162 NIETYLLEKSRAIRQARDERTFHIFYYLIAGAKEKMRSDLLLEGFNNYTFLSNGFV-PIPAAQDDEMFQETLEAMSIMGF 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  266 PPSIQQLVLQLVAGILHLGNISFCEDGNYARVESVDLLAFP--AYLLGIDSGRLQEKLTSRKMDSrwgGRsESIDVTLNV 343
Cdd:cd14921    241 SEEEQLSILKVVSSVLQLGNIVFKKERNTDQASMPDNTAAQkvCHLMGINVTDFTRSILTPRIKV---GR-DVVQKAQTK 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  344 EQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS--IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKA 421
Cdd:cd14921    317 EQADFAIEALAKATYERLFRWILTRVNKALDKTHRQGAsfLGILDIAGFEIFEVNSFEQLCINYTNEKLQQLFNHTMFIL 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  422 EQEEYVQEGIRWTPIQYFNNKVVC-DLIENKLSPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNSW---- 496
Cdd:cd14921    397 EQEEYQREGIEWNFIDFGLDLQPCiELIERPNNPPGVLALLDEECWFPKAT----DKSFVEKLCTEQGNHPKFQKPkqlk 472
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  497 -SAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPE-----KLD--------------GDKKGRP 556
Cdd:cd14921    473 dKTEFSIIHYAGKVDYNASAWLTKNMDPLNDNVTSLLNASSDKFVADLWKDvdrivGLDqmakmtesslpsasKTKKGMF 552
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  557 STAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAI 636
Cdd:cd14921    553 RTVGQLYKEQLGKLMTTLRNTTPNFVRCIIPNHEKRSGKLDAFLVLEQLRCNGVLEGIRICRQGFPNRIVFQEFRQRYEI 632
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|.
gi 1622892340  637 LTPETWPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14921    633 LAANAIPKGFMDGKQACILMIKALELDPNLYRIGQSKIFFR 673
MYSc_Myh7 cd14917
class II myosin heavy chain 7, motor domain; Myosin motor domain of beta (or slow) type I ...
32-677 5.21e-134

class II myosin heavy chain 7, motor domain; Myosin motor domain of beta (or slow) type I cardiac muscle myosin heavy chain 7 (also called CMH1, MPD1, and CMD1S). Muscle myosin is a hexameric protein containing 2 heavy chain subunits, 2 alkali light chain subunits, and 2 regulatory light chain subunits. It is expressed predominantly in normal human ventrical and in skeletal muscle tissues rich in slow-twitch type I muscle fibers. Changes in the relative abundance of this protein and the alpha (or fast) heavy subunit of cardiac myosin correlate with the contractile velocity of cardiac muscle. Its expression is also altered during thyroid hormone depletion and hemodynamic overloading. Mutations in this gene are associated with familial hypertrophic cardiomyopathy, myosin storage myopathy, dilated cardiomyopathy, and Laing early-onset distal myopathy. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276881 [Multi-domain]  Cd Length: 668  Bit Score: 422.59  E-value: 5.21e-134
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14917      2 AVLYNLKERYASWMIYTYSGLFCVTVNPYKWLPVYNAEVVAAYRGKKRSEAPPHIFSISDNAYQYMLTDRENQSILITGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVQH--------VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPD 183
Cdd:cd14917     82 SGAGKTVNTKRVIQYFAVIAAIGDRSKKdqtpgkgtLEDQIIQANPALEAFGNAKTVRNDNSSRFGKFIRIHFGATGKLA 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  184 GGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDY-YYYLNQSDTyQVDGTDDRSDFGETLSAMQV 262
Cdd:cd14917    162 SADIETYLLEKSRVIFQLKAERDYHIFYQILSNKKPELLDMLLITNNPYdYAFISQGET-TVASIDDAEELMATDNAFDV 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  263 IGIPPSIQQLVLQLVAGILHLGNISF--CEDGNYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVT 340
Cdd:cd14917    241 LGFTSEEKNSMYKLTGAIMHFGNMKFkqKQREEQAEPDGTEEADKSAYLMGLNSADLLKGLCHPRVKV----GNEYVTKG 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  341 LNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQ-EEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTL 419
Cdd:cd14917    317 QNVQQVIYATGALAKAVYEKMFNWMVTRINATLETKQpRQYFIGVLDIAGFEIFDFNSFEQLCINFTNEKLQQFFNHHMF 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  420 KAEQEEYVQEGIRWTPIQYFNNKVVC-DLIENklsPPGIMSVLDDVCATMHATgggaDQTLLQKL-QAAVGTHEHFN--- 494
Cdd:cd14917    397 VLEQEEYKKEGIEWTFIDFGMDLQACiDLIEK---PMGIMSILEEECMFPKAT----DMTFKAKLfDNHLGKSNNFQkpr 469
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  495 ----SWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGD----------KKGRP-STA 559
Cdd:cd14917    470 nikgKPEAHFSLIHYAGTVDYNIIGWLQKNKDPLNETVVGLYQKSSLKLLSNLFANYAGADapiekgkgkaKKGSSfQTV 549
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  560 GSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTP 639
Cdd:cd14917    550 SALHRENLNKLMTNLRSTHPHFVRCIIPNETKSPGVMDNPLVMHQLRCNGVLEGIRICRKGFPNRILYGDFRQRYRILNP 629
                          650       660       670
                   ....*....|....*....|....*....|....*....
gi 1622892340  640 ETWPRWRG-DERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14917    630 AAIPEGQFiDSRKGAEKLLSSLDIDHNQYKFGHTKVFFK 668
MYSc_Myo19 cd14880
class XIX myosin, motor domain; Monomeric myosin-XIX (Myo19) functions as an actin-based motor ...
37-676 1.23e-132

class XIX myosin, motor domain; Monomeric myosin-XIX (Myo19) functions as an actin-based motor for mitochondrial movement in vertebrate cells. It contains a variable number of IQ domains. Human myo19 contains a motor domain, three IQ motifs, and a short tail. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276846 [Multi-domain]  Cd Length: 658  Bit Score: 418.48  E-value: 1.23e-132
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   37 LRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREI-DLYQGAAQYEN-PPHIYALTDNMYRNM--LIDCENQCVIISGES 112
Cdd:cd14880      7 LQARYTADTFYTNAGCTLVALNPFKPVPQLYSPELmREYHAAPQPQKlKPHIFTVGEQTYRNVksLIEPVNQSIVVSGES 86
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  113 GAGKTVAAKYIMGYISKVSGG-----GNK-VQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGK 186
Cdd:cd14880     87 GAGKTWTSRCLMKFYAVVAASptsweSHKiAERIEQRILNSNPVMEAFGNACTLRNNNSSRFGKFIQLQLNRAQQMTGAA 166
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  187 ISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTyqvdgTDDRSDFGETLSAMQVIGIP 266
Cdd:cd14880    167 VQTYLLEKTRVACQAPSERNFHIFYQICKGASADERLQWHLPEGAAFSWLPNPER-----NLEEDCFEVTREAMLHLGID 241
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  267 PSIQQLVLQLVAGILHLGNISFCEDGNYARV-----ESVDLLAFPAYLLGIDSGRLQEKLTSRKMdsRWGGRSESIDVTL 341
Cdd:cd14880    242 TPTQNNIFKVLAGLLHLGNIQFADSEDEAQPcqpmdDTKESVRTSALLLKLPEDHLLETLQIRTI--RAGKQQQVFKKPC 319
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  342 NVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS--IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTL 419
Cdd:cd14880    320 SRAECDTRRDCLAKLIYARLFDWLVSVINSSICADTDSWTtfIGLLDVYGFESFPENSLEQLCINYANEKLQQHFVAHYL 399
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  420 KAEQEEYVQEGIRWTPIQYFNNKVVCDLIENklSPPGIMSVLDDVCATMHATGGGADQTLLQKLQA---AVGtHEHFnSW 496
Cdd:cd14880    400 RAQQEEYAVEGLEWSFINYQDNQTCLDLIEG--SPISICSLINEECRLNRPSSAAQLQTRIESALAgnpCLG-HNKL-SR 475
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  497 SAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP--------EKLDGDKKGRPSTAGSKIKKQAN 568
Cdd:cd14880    476 EPSFIVVHYAGPVRYHTAGLVEKNKDPVPPELTRLLQQSQDPLLQKLFPanpeektqEEPSGQSRAPVLTVVSKFKASLE 555
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  569 DLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTpetwpRWRGD 648
Cdd:cd14880    556 QLLQVLHSTTPHYIRCIKPNSQCQAQTFLQEEVLSQLEACGLVETIHISAAGFPIRVSHQNFVERYKLLR-----RLRPH 630
                          650       660
                   ....*....|....*....|....*...
gi 1622892340  649 ERQGVQHLLRAvNMEPDQYQMGSTKVFV 676
Cdd:cd14880    631 TSSGPHSPYPA-KGLSEPVHCGRTKVFM 657
MYSc_Myo41 cd14902
class XLI myosin, motor domain; The class XLI myosins are comprised of Stramenopiles. Not much ...
37-639 4.09e-132

class XLI myosin, motor domain; The class XLI myosins are comprised of Stramenopiles. Not much is known about this myosin class. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276867 [Multi-domain]  Cd Length: 716  Bit Score: 418.91  E-value: 4.09e-132
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   37 LRKRFMDDYIFTYIGSVLISVNPFKQMP-YFTDREIDLYQ--------GAAQYENPPHIYALTDNMYRNMLIDCE-NQCV 106
Cdd:cd14902      7 LSERFEHDQIYTSIGDILVALNPLKPLPdLYSESQLNAYKasmtstspVSQLSELPPHVFAIGGKAFGGLLKPERrNQSI 86
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  107 IISGESGAGKTVAAKYIMGYISKV----SGGGNKVQHVKDI---ILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRG 179
Cdd:cd14902     87 LVSGESGSGKTESTKFLMQFLTSVgrdqSSTEQEGSDAVEIgkrILQTNPILESFGNAQTIRNDNSSRFGKFIKIQFGAN 166
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  180 GEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTY----QVDGTDDRSDFGE 255
Cdd:cd14902    167 NEIVGAQIVSYLLEKVRLLHQSPEERSFHIFYELLEGADKTLLDLLGLQKGGKYELLNSYGPSfarkRAVADKYAQLYVE 246
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  256 TLSAMQVIGIPPSIQQLVLQLVAGILHLGNISFC-----EDGNYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrw 330
Cdd:cd14902    247 TVRAFEDTGVGELERLDIFKILAALLHLGNVNFTaengqEDATAVTAASRFHLAKCAELMGVDVDKLETLLSSREIKA-- 324
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  331 gGRsESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAM----------QKPQEEYSIGVLDIYGFEIFQKNGFEQ 400
Cdd:cd14902    325 -GV-EVMVLKLTPEQAKEICGSLAKAIYGRLFTWLVRRLSDEInyfdsavsisDEDEELATIGILDIFGFESLNRNGFEQ 402
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  401 FCINFVNEKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHatggGADQTLL 480
Cdd:cd14902    403 LCINYANERLQAQFNEFVFVKEQQIYIAEGIDWKNISYPSNAACLALFDDK--SNGLFSLLDQECLMPK----GSNQALS 476
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  481 QKLQAAVGTHEHfnswsagFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKKGRPSTAG 560
Cdd:cd14902    477 TKFYRYHGGLGQ-------FVVHHFAGRVCYNVEQFVEKNTDALPADASDILSSSSNEVVVAIGADENRDSPGADNGAAG 549
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  561 SK-------------IKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQF 627
Cdd:cd14902    550 RRrysmlrapsvsaqFKSQLDRLIVQIGRTEAHYVRCLKPNEVKKPGIFDRERMVEQMRSVGVLEAVRIARHGYSVRLAH 629
                          650
                   ....*....|..
gi 1622892340  628 AKFLQRYAILTP 639
Cdd:cd14902    630 ASFIELFSGFKC 641
MYSc_Myo17 cd14879
class XVII myosin, motor domain; This fungal myosin which is also known as chitin synthase ...
28-676 1.04e-131

class XVII myosin, motor domain; This fungal myosin which is also known as chitin synthase uses its motor domain to tether its vesicular cargo to peripheral actin. It works in opposition to dynein, contributing to the retention of Mcs1 vesicles at the site of cell growth and increasing vesicle fusion necessary for polarized growth. Class 17 myosins consist of a N-terminal myosin motor domain with Cyt-b5, chitin synthase 2, and a DEK_C domains at it C-terminus. The chitin synthase region contains several transmembrane domains by which myosin 17 is thought to bind secretory vesicles. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276845 [Multi-domain]  Cd Length: 647  Bit Score: 415.41  E-value: 1.04e-131
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   28 ITEDAIAANLRKRFMDDYIFTYIGS-VLISVNPFKQMPYFTDreidlyQGAAQYEN-------------PPHIYALTDNM 93
Cdd:cd14879      1 PSDDAITSHLASRFRSDLPYTRLGSsALVAVNPYKYLSSNSD------ASLGEYGSeyydttsgskeplPPHAYDLAARA 74
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   94 YRNMLIDCENQCVIISGESGAGKTVAAKYIMGYISKVSGGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFE 173
Cdd:cd14879     75 YLRMRRRSEDQAVVFLGETGSGKSESRRLLLRQLLRLSSHSKKGTKLSSQISAAEFVLDSFGNAKTLTNPNASRFGRYTE 154
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  174 IQFSRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVD---GTDDR 250
Cdd:cd14879    155 LQFNERGRLIGAKVLDYRLERSRVASVPTGERNFHVFYYLLAGASPEERQHLGLDDPSDYALLASYGCHPLPlgpGSDDA 234
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  251 SDFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISFCED--GNY--ARVESVDLLAFPAYLLGIDSGRLQEKLTSR-K 325
Cdd:cd14879    235 EGFQELKTALKTLGFKRKHVAQICQLLAAILHLGNLEFTYDheGGEesAVVKNTDVLDIVAAFLGVSPEDLETSLTYKtK 314
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  326 MDSRwggrsESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS--IGVLDIYGFEIF---QKNGFEQ 400
Cdd:cd14879    315 LVRK-----ELCTVFLDPEGAAAQRDELARTLYSLLFAWVVETINQKLCAPEDDFAtfISLLDFPGFQNRsstGGNSLDQ 389
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  401 FCINFVNEKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMhatGGGADQTLL 480
Cdd:cd14879    390 FCVNFANERLHNYVLRSFFERKAEELEAEGVSVPATSYFDNSDCVRLLRGK--PGGLLGILDDQTRRM---PKKTDEQML 464
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  481 QKLQAAVGTHEHF--------NSWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQaflrmlFPEKLDgdk 552
Cdd:cd14879    465 EALRKRFGNHSSFiavgnfatRSGSASFTVNHYAGEVTYSVEGFLERNGDVLSPDFVNLLRGATQ------LNAALS--- 535
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  553 kgrpstagskikkqanDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQ 632
Cdd:cd14879    536 ----------------ELLDTLDRTRLWSVFCIRPNDSQLPNSFDKRRVKAQIRSLGLPELAARLRVEYVVSLEHAEFCE 599
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|....
gi 1622892340  633 RYAILTPETwprwrgDERQGVQHLLRAVNMEPDQYQMGSTKVFV 676
Cdd:cd14879    600 RYKSTLRGS------AAERIRQCARANGWWEGRDYVLGNTKVFL 637
MYSc_Myh14_mammals cd14930
class II myosin heavy chain 14 motor domain; Myosin motor domain of non-muscle myosin heavy ...
32-677 1.09e-131

class II myosin heavy chain 14 motor domain; Myosin motor domain of non-muscle myosin heavy chain 14 (also called FLJ13881, KIAA2034, MHC16, MYH17). Its members include mammals, chickens, and turtles. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. Some of the data used for this classification were produced by the CyMoBase team at the Max-Planck-Institute for Biophysical Chemistry. The sequence names are composed of the species abbreviation followed by the protein abbreviation and optional protein classifier and variant designations.


Pssm-ID: 276893 [Multi-domain]  Cd Length: 670  Bit Score: 416.42  E-value: 1.09e-131
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14930      2 SVLHNLRERYYSGLIYTYSGLFCVVINPYKQLPIYTEAIVEMYRGKKRHEVPPHVYAVTEGAYRSMLQDREDQSILCTGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGG--GNKVQHV----KDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGG 185
Cdd:cd14930     82 SGAGKTENTKKVIQYLAHVASSpkGRKEPGVpgelERQLLQANPILEAFGNAKTVKNDNSSRFGKFIRINFDVAGYIVGA 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  186 KISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDgtDDRSDFGETLSAMQVIGI 265
Cdd:cd14930    162 NIETYLLEKSRAIRQAKDECSFHIFYQLLGGAGEQLKADLLLEPCSHYRFLTNGPSSSPG--QERELFQETLESLRVLGF 239
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  266 PPSIQQLVLQLVAGILHLGNISFCEDGNYARVESVDLLAFPAY--LLGIDSGRLQEKLTSRKMDSrwgGRsESIDVTLNV 343
Cdd:cd14930    240 SHEEITSMLRMVSAVLQFGNIVLKRERNTDQATMPDNTAAQKLcrLLGLGVTDFSRALLTPRIKV---GR-DYVQKAQTK 315
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  344 EQAAYTRDALAKGLYARLFDFLVEAINRAMQK-PQEEYS-IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKA 421
Cdd:cd14930    316 EQADFALEALAKATYERLFRWLVLRLNRALDRsPRQGASfLGILDIAGFEIFQLNSFEQLCINYTNEKLQQLFNHTMFVL 395
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  422 EQEEYVQEGIRWTPIQYFNNKVVC-DLIENKLSPPGIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNSW---- 496
Cdd:cd14930    396 EQEEYQREGIPWTFLDFGLDLQPCiDLIERPANPPGLLALLDEECWFPKAT----DKSFVEKVAQEQGGHPKFQRPrhlr 471
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  497 -SAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP--------EKL----DGDKKGRP-----ST 558
Cdd:cd14930    472 dQADFSVLHYAGKVDYKANEWLMKNMDPLNDNVAALLHQSTDRLTAEIWKdvegivglEQVsslgDGPPGGRPrrgmfRT 551
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  559 AGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILT 638
Cdd:cd14930    552 VGQLYKESLSRLMATLSNTNPSFVRCIVPNHEKRAGKLEPRLVLDQLRCNGVLEGIRICRQGFPNRILFQEFRQRYEILT 631
                          650       660       670
                   ....*....|....*....|....*....|....*....
gi 1622892340  639 PETWPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14930    632 PNAIPKGFMDGKQACEKMIQALELDPNLYRVGQSKIFFR 670
MYSc_Myh6 cd14916
class II myosin heavy chain 6, motor domain; Myosin motor domain of alpha (or fast) cardiac ...
32-677 1.54e-129

class II myosin heavy chain 6, motor domain; Myosin motor domain of alpha (or fast) cardiac muscle myosin heavy chain 6. Cardiac muscle myosin is a hexamer consisting of two heavy chain subunits, two light chain subunits, and two regulatory subunits. This gene encodes the alpha heavy chain subunit of cardiac myosin. Mutations in this gene cause familial hypertrophic cardiomyopathy and atrial septal defect. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276880 [Multi-domain]  Cd Length: 670  Bit Score: 410.60  E-value: 1.54e-129
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14916      2 AVLYNLKERYAAWMIYTYSGLFCVTVNPYKWLPVYNAEVVAAYRGKKRSEAPPHIFSISDNAYQYMLTDRENQSILITGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVQH---------VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEP 182
Cdd:cd14916     82 SGAGKTVNTKRVIQYFASIAAIGDRSKKenpnankgtLEDQIIQANPALEAFGNAKTVRNDNSSRFGKFIRIHFGATGKL 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  183 DGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDY-YYYLNQSDTyQVDGTDDRSDFGETLSAMQ 261
Cdd:cd14916    162 ASADIETYLLEKSRVIFQLKAERNYHIFYQILSNKKPELLDMLLVTNNPYdYAFVSQGEV-SVASIDDSEELLATDSAFD 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  262 VIGIPPSIQQLVLQLVAGILHLGNISFCEDGNYARVE--SVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDV 339
Cdd:cd14916    241 VLGFTAEEKAGVYKLTGAIMHYGNMKFKQKQREEQAEpdGTEDADKSAYLMGLNSADLLKGLCHPRVKV----GNEYVTK 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  340 TLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQ-EEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELT 418
Cdd:cd14916    317 GQSVQQVYYSIGALAKSVYEKMFNWMVTRINATLETKQpRQYFIGVLDIAGFEIFDFNSFEQLCINFTNEKLQQFFNHHM 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  419 LKAEQEEYVQEGIRWTPIQYFNNKVVC-DLIEnklSPPGIMSVLDDVCATMHATgggaDQTLLQKL-QAAVGTHEHFN-- 494
Cdd:cd14916    397 FVLEQEEYKKEGIEWEFIDFGMDLQACiDLIE---KPMGIMSILEEECMFPKAS----DMTFKAKLyDNHLGKSNNFQkp 469
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  495 -----SWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKKGRPSTAGSKIKKQA-- 567
Cdd:cd14916    470 rnvkgKQEAHFSLVHYAGTVDYNILGWLEKNKDPLNETVVGLYQKSSLKLMATLFSTYASADTGDSGKGKGGKKKGSSfq 549
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  568 ----------NDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAIL 637
Cdd:cd14916    550 tvsalhrenlNKLMTNLKTTHPHFVRCIIPNERKAPGVMDNPLVMHQLRCNGVLEGIRICRKGFPNRILYGDFRQRYRIL 629
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|.
gi 1622892340  638 TPETWPRWRG-DERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14916    630 NPAAIPEGQFiDSRKGAEKLLGSLDIDHNQYKFGHTKVFFK 670
MYSc_Myo25 cd14886
class XXV myosin, motor domain; These myosins are MyTH-FERM myosins that play a role in cell ...
37-677 7.63e-129

class XXV myosin, motor domain; These myosins are MyTH-FERM myosins that play a role in cell adhesion and filopodia formation. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276851  Cd Length: 650  Bit Score: 408.12  E-value: 7.63e-129
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   37 LRKRFMDDYIFTYIGSVLISVNPFKQMP-YFTDREIDLYQGAAQY-----ENPPHIYALTDNMYRNMLIDCENQCVIISG 110
Cdd:cd14886      7 LRDRFAKDKIYTYAGKLLVALNPFKQIRnLYGTEVIGRYRQADTSrgfpsDLPPHSYAVAQSALNGLISDGISQSCIVSG 86
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  111 ESGAGKTVAAKYIMGYISKV-SGGGNKVQHVkdiILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISN 189
Cdd:cd14886     87 ESGAGKTETAKQLMNFFAYGhSTSSTDVQSL---ILGSNPLLESFGNAKTLRNNNSSRFGKFIKLLVGPDGGLKGGKITS 163
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  190 FLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSI 269
Cdd:cd14886    164 YMLELSRIEFQSTNERNYHIFYQCIKGLSPEEKKSLGFKSLESYNFLNASKCYDAPGIDDQKEFAPVRSQLEKLFSKNEI 243
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  270 QQLvLQLVAGILHLGNISFCEDG-----NYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNVE 344
Cdd:cd14886    244 DSF-YKCISGILLAGNIEFSEEGdmgviNAAKISNDEDFGKMCELLGIESSKAAQAIITKVVVI----NNETIISPVTQA 318
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  345 QAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS-IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQ 423
Cdd:cd14886    319 QAEVNIRAVAKDLYGALFELCVDTLNEIIQFDADARPwIGILDIYGFEFFERNTYEQLLINYANERLQQYFINQVFKSEI 398
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  424 EEYVQEGIRWTPIQYFNNKVVCDLIENklspP--GIMSVLDDVCatMHATGGGadqtllQKLQAAVGTHEHFNSWSAG-- 499
Cdd:cd14886    399 QEYEIEGIDHSMITFTDNSNVLAVFDK----PnlSIFSFLEEQC--LIQTGSS------EKFTSSCKSKIKNNSFIPGkg 466
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  500 ----FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPE--KLDGDKKGRpsTAGSKIKKQANDLVAT 573
Cdd:cd14886    467 sqcnFTIVHTAATVTYNTEEFVDKNKHKLSVDILELLMGSTNPIVNKAFSDipNEDGNMKGK--FLGSTFQLSIDQLMKT 544
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  574 LMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWRG--DERQ 651
Cdd:cd14886    545 LSATKSHFIRCIKTNQDKVPNKYETKSVYNQLISLSIFESIQTIHRGFAYNDTFEEFFHRNKILISHNSSSQNAgeDLVE 624
                          650       660
                   ....*....|....*....|....*.
gi 1622892340  652 GVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14886    625 AVKSILENLGIPCSDYRIGKTKVFLR 650
MYSc_Myh2_mammals cd14912
class II myosin heavy chain 2, motor domain; Myosin motor domain of type IIa skeletal muscle ...
32-677 2.26e-128

class II myosin heavy chain 2, motor domain; Myosin motor domain of type IIa skeletal muscle myosin heavy chain 2 (also called MYH2A, MYHSA2, MyHC-IIa, MYHas8, MyHC-2A) in mammals. Mutations in this gene results in inclusion body myopathy-3 and familial congenital myopathy. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276877 [Multi-domain]  Cd Length: 673  Bit Score: 407.58  E-value: 2.26e-128
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14912      2 AVLYNLKERYAAWMIYTYSGLFCVTVNPYKWLPVYNPEVVTAYRGKKRQEAPPHIFSISDNAYQFMLTDRENQSILITGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVQH----------VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGE 181
Cdd:cd14912     82 SGAGKTVNTKRVIQYFATIAVTGEKKKEeitsgkmqgtLEDQIISANPLLEAFGNAKTVRNDNSSRFGKFIRIHFGTTGK 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  182 PDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQ 261
Cdd:cd14912    162 LASADIETYLLEKSRVTFQLKAERSYHIFYQITSNKKPELIEMLLITTNPYDYPFVSQGEISVASIDDQEELMATDSAID 241
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  262 VIGIPPSIQQLVLQLVAGILHLGNISFCEDGNYARVE--SVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDV 339
Cdd:cd14912    242 ILGFTNEEKVSIYKLTGAVMHYGNLKFKQKQREEQAEpdGTEVADKAAYLQSLNSADLLKALCYPRVKV----GNEYVTK 317
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  340 TLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQ-EEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELT 418
Cdd:cd14912    318 GQTVEQVTNAVGALAKAVYEKMFLWMVARINQQLDTKQpRQYFIGVLDIAGFEIFDFNSLEQLCINFTNEKLQQFFNHHM 397
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  419 LKAEQEEYVQEGIRWTPIQYFNNKVVC-DLIENklsPPGIMSVLDDVCATMHATGGG-----ADQTL-----LQKLQAAV 487
Cdd:cd14912    398 FVLEQEEYKKEGIEWTFIDFGMDLAACiELIEK---PMGIFSILEEECMFPKATDTSfknklYEQHLgksanFQKPKVVK 474
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  488 GTHEhfnswsAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP-------------EKLDGDKKG 554
Cdd:cd14912    475 GKAE------AHFSLIHYAGVVDYNITGWLDKNKDPLNETVVGLYQKSAMKTLAYLFSgaqtaegasagggAKKGGKKKG 548
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  555 RP-STAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQR 633
Cdd:cd14912    549 SSfQTVSALFRENLNKLMTNLRSTHPHFVRCIIPNETKTPGAMEHELVLHQLRCNGVLEGIRICRKGFPSRILYADFKQR 628
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|....*
gi 1622892340  634 YAILTPETWPRWRG-DERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14912    629 YKVLNASAIPEGQFiDSKKASEKLLASIDIDHTQYKFGHTKVFFK 673
MYSc_Myh8 cd14918
class II myosin heavy chain 8, motor domain; Myosin motor domain of perinatal skeletal muscle ...
36-677 2.29e-126

class II myosin heavy chain 8, motor domain; Myosin motor domain of perinatal skeletal muscle myosin heavy chain 8 (also called MyHC-peri, MyHC-pn). Myosin is a hexameric protein composed of a pair of myosin heavy chains (MYH) and two pairs of nonidentical light chains. A mutation in this gene results in trismus-pseudocamptodactyly syndrome. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276882 [Multi-domain]  Cd Length: 668  Bit Score: 402.19  E-value: 2.29e-126
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGAG 115
Cdd:cd14918      6 NLKERYAAWMIYTYSGLFCVTVNPYKWLPVYNPEVVAAYRGKKRQEAPPHIFSISDNAYQFMLTDRENQSILITGESGAG 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  116 KTVAAKYIMGYISKVSGGGNKVQH--------VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKI 187
Cdd:cd14918     86 KTVNTKRVIQYFATIAVTGEKKKEesgkmqgtLEDQIISANPLLEAFGNAKTVRNDNSSRFGKFIRIHFGTTGKLASADI 165
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  188 SNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPP 267
Cdd:cd14918    166 ETYLLEKSRVTFQLKAERSYHIFYQITSNKKPDLIEMLLITTNPYDYAFVSQGEITVPSIDDQEELMATDSAIDILGFTP 245
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  268 SIQQLVLQLVAGILHLGNISFCEDGNYARVE--SVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVTLNVEQ 345
Cdd:cd14918    246 EEKVSIYKLTGAVMHYGNMKFKQKQREEQAEpdGTEVADKAAYLQSLNSADLLKALCYPRVKV----GNEYVTKGQTVQQ 321
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  346 AAYTRDALAKGLYARLFDFLVEAINRAMQKPQ-EEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQE 424
Cdd:cd14918    322 VYNAVGALAKAVYEKMFLWMVTRINQQLDTKQpRQYFIGVLDIAGFEIFDFNSLEQLCINFTNEKLQQFFNHHMFVLEQE 401
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  425 EYVQEGIRWTPIQYFNNKVVC-DLIENklsPPGIMSVLDDVCATMHATGGG-----ADQTL-----LQKLQAAVGTHEhf 493
Cdd:cd14918    402 EYKKEGIEWTFIDFGMDLAACiELIEK---PLGIFSILEEECMFPKATDTSfknklYDQHLgksanFQKPKVVKGKAE-- 476
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  494 nswsAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLF----------PEKLDGDKKGRP-STAGSK 562
Cdd:cd14918    477 ----AHFSLIHYAGTVDYNITGWLDKNKDPLNDTVVGLYQKSAMKTLASLFstyasaeadsGAKKGAKKKGSSfQTVSAL 552
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  563 IKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETW 642
Cdd:cd14918    553 FRENLNKLMTNLRSTHPHFVRCIIPNETKTPGAMEHELVLHQLRCNGVLEGIRICRKGFPSRILYGDFKQRYKVLNASAI 632
                          650       660       670
                   ....*....|....*....|....*....|....*.
gi 1622892340  643 PRWRG-DERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14918    633 PEGQFiDSKKASEKLLASIDIDHTQYKFGHTKVFFK 668
MYSc_Myh1_mammals cd14910
class II myosin heavy chain 1, motor domain; Myosin motor domain of type IIx skeletal muscle ...
32-677 2.15e-125

class II myosin heavy chain 1, motor domain; Myosin motor domain of type IIx skeletal muscle myosin heavy chain 1 (also called MYHSA1, MYHa, MyHC-2X/D, MGC133384) in mammals. Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276875 [Multi-domain]  Cd Length: 671  Bit Score: 399.88  E-value: 2.15e-125
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14910      2 AVLYNLKERYAAWMIYTYSGLFCVTVNPYKWLPVYNAEVVTAYRGKKRQEAPPHIFSISDNAYQFMLTDRENQSILITGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVQH----------VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGE 181
Cdd:cd14910     82 SGAGKTVNTKRVIQYFATIAVTGEKKKEeatsgkmqgtLEDQIISANPLLEAFGNAKTVRNDNSSRFGKFIRIHFGTTGK 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  182 PDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQ 261
Cdd:cd14910    162 LASADIETYLLEKSRVTFQLKAERSYHIFYQIMSNKKPDLIEMLLITTNPYDYAFVSQGEITVPSIDDQEELMATDSAIE 241
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  262 VIGIPPSIQQLVLQLVAGILHLGNISFCEDGNYARVE--SVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDV 339
Cdd:cd14910    242 ILGFTSDERVSIYKLTGAVMHYGNMKFKQKQREEQAEpdGTEVADKAAYLQNLNSADLLKALCYPRVKV----GNEYVTK 317
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  340 TLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQ-EEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELT 418
Cdd:cd14910    318 GQTVQQVYNAVGALAKAVYDKMFLWMVTRINQQLDTKQpRQYFIGVLDIAGFEIFDFNSLEQLCINFTNEKLQQFFNHHM 397
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  419 LKAEQEEYVQEGIRWTPIQYFNNKVVC-DLIENklsPPGIMSVLDDVCATMHATgggaDQTLLQKL-QAAVGTHEHFN-- 494
Cdd:cd14910    398 FVLEQEEYKKEGIEWEFIDFGMDLAACiELIEK---PMGIFSILEEECMFPKAT----DTSFKNKLyEQHLGKSNNFQkp 470
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  495 -----SWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP-----------EKLDGDKKGRP-S 557
Cdd:cd14910    471 kpakgKVEAHFSLIHYAGTVDYNIAGWLDKNKDPLNETVVGLYQKSSMKTLALLFSgaaaaeaeeggGKKGGKKKGSSfQ 550
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  558 TAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAIL 637
Cdd:cd14910    551 TVSALFRENLNKLMTNLRSTHPHFVRCIIPNETKTPGAMEHELVLHQLRCNGVLEGIRICRKGFPSRILYADFKQRYKVL 630
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|.
gi 1622892340  638 TPETWPRWRG-DERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14910    631 NASAIPEGQFiDSKKASEKLLGSIDIDHTQYKFGHTKVFFK 671
MYSc_Myo16 cd14878
class XVI myosin, motor domain; These XVI type myosins are also known as Neuronal ...
37-677 2.66e-125

class XVI myosin, motor domain; These XVI type myosins are also known as Neuronal tyrosine-phosphorylated phosphoinositide-3-kinase adapter 3/NYAP3. Myo16 is thought to play a regulatory role in cell cycle progression and has been recently implicated in Schizophrenia. Class XVI myosins are characterized by an N-terminal ankyrin repeat domain and some with chitin synthase domains that arose independently from the ones in the class XVII fungal myosins. They bind protein phosphatase 1 catalytic subunits 1alpha/PPP1CA and 1gamma/PPP1CC. Human Myo16 interacts with ACOT9, ARHGAP26 and PIK3R2 and with components of the WAVE1 complex, CYFIP1 and NCKAP1. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276844 [Multi-domain]  Cd Length: 656  Bit Score: 398.80  E-value: 2.66e-125
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   37 LRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLY---QGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESG 113
Cdd:cd14878      7 IQKRFGNNQIYTFIGDILLLVNPYKELPIYSTMVSQLYlssSGQLCSSLPPHLFSCAERAFHQLFQERRPQCFILSGERG 86
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  114 AGKTVAAKYIMGYISKVSGGG-----NKVQHVkdiilqsNPLLEAFGNAKTVRNNNSSRFGKYFEIQF-SRGGEPDGGKI 187
Cdd:cd14878     87 SGKTEASKQIMKHLTCRASSSrttfdSRFKHV-------NCILEAFGHAKTTLNDLSSCFIKYFELQFcERKKHLTGARI 159
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  188 SNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQS---DTYQVDGTDDRSDFGETLSAMQVIG 264
Cdd:cd14878    160 YTYMLEKSRLVSQPPGQSNFLIFYLLMDGLSAEEKYGLHLNNLCAHRYLNQTmreDVSTAERSLNREKLAVLKQALNVVG 239
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  265 IPPSIQQLVLQLVAGILHLGNISFC--EDGNYARVESVDLLAFPAYLLGIDSGRLQEKLTSrkmDSRWGgRSESIDVTLN 342
Cdd:cd14878    240 FSSLEVENLFVILSAILHLGDIRFTalTEADSAFVSDLQLLEQVAGMLQVSTDELASALTT---DIQYF-KGDMIIRRHT 315
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  343 VEQAAYTRDALAKGLYARLFDFLVEAINRAMQKpQEEYS------IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIE 416
Cdd:cd14878    316 IQIAEFYRDLLAKSLYSRLFSFLVNTVNCCLQS-QDEQKsmqtldIGILDIFGFEEFQKNEFEQLCVNMTNEKMHHYINE 394
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  417 LTLKAEQEEYVQEGIRWTPIQYFNNKV-VCDLIENKlsPPGIMSVLDDVCATMHAtgggADQTLLQKLQAAVGTHEH--- 492
Cdd:cd14878    395 VLFLQEQTECVQEGVTMETAYSPGNQTgVLDFFFQK--PSGFLSLLDEESQMIWS----VEPNLPKKLQSLLESSNTnav 468
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  493 ------------FNSWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLdgdkkgrpSTAG 560
Cdd:cd14878    469 yspmkdgngnvaLKDQGTAFTVMHYAGRVMYEIVGAIEKNKDSLSQNLLFVMKTSENVVINHLFQSKL--------VTIA 540
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  561 SKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTpE 640
Cdd:cd14878    541 SQLRKSLADIIGKLQKCTPHFIHCIKPNNSKLPDTFDNFYVSAQLQYIGVLEMVKIFRYGYPVRLSFSDFLSRYKPLA-D 619
                          650       660       670
                   ....*....|....*....|....*....|....*....
gi 1622892340  641 TWPrwRGDERQGVQHLLRAVNMEPDQ--YQMGSTKVFVK 677
Cdd:cd14878    620 TLL--GEKKKQSAEERCRLVLQQCKLqgWQMGVRKVFLK 656
MYSc_Myh4 cd14915
class II myosin heavy chain 4, motor domain; Myosin motor domain of skeletal muscle myosin ...
32-677 9.26e-125

class II myosin heavy chain 4, motor domain; Myosin motor domain of skeletal muscle myosin heavy chain 4 (also called MYH2B, MyHC-2B, MyHC-IIb). Class II myosins, also called conventional myosins, are the myosin type responsible for producing actomyosin contraction in metazoan muscle and non-muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276879 [Multi-domain]  Cd Length: 671  Bit Score: 397.95  E-value: 9.26e-125
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14915      2 AVLYNLKERYAAWMIYTYSGLFCVTVNPYKWLPVYNPEVVTAYRGKKRQEAPPHIFSISDNAYQFMLTDRENQSILITGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVQH----------VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGE 181
Cdd:cd14915     82 SGAGKTVNTKRVIQYFATIAVTGEKKKEeaasgkmqgtLEDQIISANPLLEAFGNAKTVRNDNSSRFGKFIRIHFGATGK 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  182 PDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDY-YYYLNQSDTyQVDGTDDRSDFGETLSAM 260
Cdd:cd14915    162 LASADIETYLLEKSRVTFQLKAERSYHIFYQIMSNKKPELIEMLLITTNPYdFAFVSQGEI-TVPSIDDQEELMATDSAV 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  261 QVIGIPPSIQQLVLQLVAGILHLGNISFCEDGNYARVE--SVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESID 338
Cdd:cd14915    241 DILGFSADEKVAIYKLTGAVMHYGNMKFKQKQREEQAEpdGTEVADKAAYLTSLNSADLLKALCYPRVKV----GNEYVT 316
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  339 VTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQ-EEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIEL 417
Cdd:cd14915    317 KGQTVQQVYNSVGALAKAIYEKMFLWMVTRINQQLDTKQpRQYFIGVLDIAGFEIFDFNSLEQLCINFTNEKLQQFFNHH 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  418 TLKAEQEEYVQEGIRWTPIQYFNNKVVC-DLIENklsPPGIMSVLDDVCATMHATGGGADQTL----------LQKLQAA 486
Cdd:cd14915    397 MFVLEQEEYKKEGIEWEFIDFGMDLAACiELIEK---PMGIFSILEEECMFPKATDTSFKNKLyeqhlgksnnFQKPKPA 473
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  487 VGTHEhfnswsAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP-----------EKLDGDKKGR 555
Cdd:cd14915    474 KGKAE------AHFSLVHYAGTVDYNIAGWLDKNKDPLNETVVGLYQKSGMKTLAFLFSggqtaeaegggGKKGGKKKGS 547
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  556 P-STAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRY 634
Cdd:cd14915    548 SfQTVSALFRENLNKLMTNLRSTHPHFVRCLIPNETKTPGAMEHELVLHQLRCNGVLEGIRICRKGFPSRILYADFKQRY 627
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|....
gi 1622892340  635 AILTPETWPRWRG-DERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14915    628 KVLNASAIPEGQFiDSKKASEKLLGSIDIDHTQYKFGHTKVFFK 671
MYSc_Myh13 cd14923
class II myosin heavy chain 13, motor domain; Myosin motor domain of skeletal muscle myosin ...
32-677 3.07e-124

class II myosin heavy chain 13, motor domain; Myosin motor domain of skeletal muscle myosin heavy chain 13 (also called MyHC-eo) in mammals, chicken, and green anole. Myh13 is a myosin whose expression is restricted primarily to the extrinsic eye muscles which are specialized for function in eye movement. Class II myosins, also called conventional myosins, are the myosin type responsible for producing muscle contraction in muscle cells. Myosin II contains two heavy chains made up of the head (N-terminal) and tail (C-terminal) domains with a coiled-coil morphology that holds the two heavy chains together. The intermediate neck domain is the region creating the angle between the head and tail. It also contains 4 light chains which bind the heavy chains in the "neck" region between the head and tail. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. Class-II myosins are regulated by phosphorylation of the myosin light chain or by binding of Ca2+. A cyclical interaction between myosin and actin provides the driving force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276887 [Multi-domain]  Cd Length: 671  Bit Score: 396.75  E-value: 3.07e-124
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGE 111
Cdd:cd14923      2 AVLYNLKERYAAWMIYTYSGLFCVTVNPYKWLPVYNPEVVAAYRGKKRQEAPPHIFSISDNAYQFMLTDRDNQSILITGE 81
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  112 SGAGKTVAAKYIMGYISKVSGGGNKVQH---------VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEP 182
Cdd:cd14923     82 SGAGKTVNTKRVIQYFATIAVTGDKKKEqqpgkmqgtLEDQIIQANPLLEAFGNAKTVRNDNSSRFGKFIRIHFGATGKL 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  183 DGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQV 262
Cdd:cd14923    162 ASADIETYLLEKSRVTFQLSSERSYHIFYQIMSNKKPELIDLLLISTNPFDFPFVSQGEVTVASIDDSEELLATDNAIDI 241
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  263 IGIPPSIQQLVLQLVAGILHLGNISFCEDGNYARVE--SVDLLAFPAYLLGIDSGRLQEKLTSRKMDSrwggRSESIDVT 340
Cdd:cd14923    242 LGFSSEEKVGIYKLTGAVMHYGNMKFKQKQREEQAEpdGTEVADKAGYLMGLNSAEMLKGLCCPRVKV----GNEYVTKG 317
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  341 LNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQ-EEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTL 419
Cdd:cd14923    318 QNVQQVTNSVGALAKAVYEKMFLWMVTRINQQLDTKQpRQYFIGVLDIAGFEIFDFNSLEQLCINFTNEKLQQFFNHHMF 397
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  420 KAEQEEYVQEGIRWTPIQYFNNKVVC-DLIENklsPPGIMSVLDDVCATMHATGGG-----ADQTL-----LQKLQAAVG 488
Cdd:cd14923    398 VLEQEEYKKEGIEWEFIDFGMDLAACiELIEK---PMGIFSILEEECMFPKATDTSfknklYDQHLgksnnFQKPKPAKG 474
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  489 THEhfnswsAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFP------------EKLDGDKKGRP 556
Cdd:cd14923    475 KAE------AHFSLVHYAGTVDYNIAGWLDKNKDPLNETVVGLYQKSSLKLLSFLFSnyagaeagdsggSKKGGKKKGSS 548
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  557 -STAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYA 635
Cdd:cd14923    549 fQTVSAVFRENLNKLMTNLRSTHPHFVRCLIPNETKTPGVMDHYLVMHQLRCNGVLEGIRICRKGFPSRILYADFKQRYR 628
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|...
gi 1622892340  636 ILTPETWPRWRG-DERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14923    629 ILNASAIPEGQFiDSKNASEKLLNSIDVDREQYRFGHTKVFFK 671
MYSc_Myo13 cd14875
class XIII myosin, motor domain; These myosins have an N-terminal motor domain, a light-chain ...
47-677 5.41e-118

class XIII myosin, motor domain; These myosins have an N-terminal motor domain, a light-chain binding domain, and a C-terminal GPA/Q-rich domain. There is little known about the function of this myosin class. Two of the earliest members identified in this class are green alga Acetabularia cliftonii, Aclmyo1 and Aclmyo2. They are striking with their short tail of Aclmyo1 of 18 residues and the maximum of 7 IQ motifs in Aclmyo2. It is thought that these myosins are involved in organelle transport and tip growth. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276842 [Multi-domain]  Cd Length: 664  Bit Score: 379.54  E-value: 5.41e-118
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   47 FTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYEN-PPHIYALTDNMYRNMLI-DCENQCVIISGESGAGKTVAAKYIM 124
Cdd:cd14875     18 YSLMGEMVLSVNPFRLMPFNSEEERKKYLALPDPRLlPPHIWQVAHKAFNAIFVqGLGNQSVVISGESGSGKTENAKMLI 97
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  125 GYISKVS--GGGNKVQH-----VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQF-SRGGEPDGGKISNFLLEKSR 196
Cdd:cd14875     98 AYLGQLSymHSSNTSQRsiadkIDENLKWSNPVMESFGNARTVRNDNSSRFGKYIKLYFdPTSGVMVGGQTVTYLLEKSR 177
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  197 VVMQNENERNFHIYYQLLEGASQEQRQNLG-LMTPDYYYYLNQSDTYQ---VDGT--DDRSDFGETLSAMQVIGIPPSIQ 270
Cdd:cd14875    178 IIMQSPGERNYHIFYEMLAGLSPEEKKELGgLKTAQDYKCLNGGNTFVrrgVDGKtlDDAHEFQNVRHALSMIGVELETQ 257
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  271 QLVLQLVAGILHLGNISFCEDGN-YARVESVDLLAFPAYLLGIDSGRLQEKLTSRKmdsrwggRSESIDVTLNVEQAAYT 349
Cdd:cd14875    258 NSIFRVLASILHLMEVEFESDQNdKAQIADETPFLTACRLLQLDPAKLRECFLVKS-------KTSLVTILANKTEAEGF 330
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  350 RDALAKGLYARLFDFLVEAINRAMQkPQEEYS----IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEE 425
Cdd:cd14875    331 RNAFCKAIYVGLFDRLVEFVNASIT-PQGDCSgckyIGLLDIFGFENFTRNSFEQLCINYANESLQNHYNKYTFINDEEE 409
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  426 YVQEGIRWTPIQYFNNKVVCDLIENKLSppGIMSVLDDVCatmHATGGGADQTllqklqaavgTHEHFNSWSA------- 498
Cdd:cd14875    410 CRREGIQIPKIEFPDNSECVNMFDQKRT--GIFSMLDEEC---NFKGGTTERF----------TTNLWDQWANkspyfvl 474
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  499 -------GFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKkgRPSTAGSKIKKQANDLV 571
Cdd:cd14875    475 pkstipnQFGVNHYAAFVNYNTDEWLEKNTDALKEDMYECVSNSTDEFIRTLLSTEKGLAR--RKQTVAIRFQRQLTDLR 552
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  572 ATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRW--RGDE 649
Cdd:cd14875    553 TELESTETQFIRCIKPNMEASPSFLDNLLVGSQLESAGVLQTIALKRQGYPVRRPIEQFCRYFYLIMPRSTASLfkQEKY 632
                          650       660       670
                   ....*....|....*....|....*....|..
gi 1622892340  650 RQGVQHLL----RAVNMEPDQYQMGSTKVFVK 677
Cdd:cd14875    633 SEAAKDFLayyqRLYGWAKPNYAVGKTKVFLR 664
MYSc_Myo24A cd14937
class XXIV A myosin, motor domain; These myosins have a 1-2 IQ motifs in their neck and a ...
40-677 1.46e-107

class XXIV A myosin, motor domain; These myosins have a 1-2 IQ motifs in their neck and a coiled-coil region in their C-terminal tail. The function of the class XXIV myosins remain elusive. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276897  Cd Length: 637  Bit Score: 350.85  E-value: 1.46e-107
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   40 RFMDDYIFTYIGSVLISVNPFKQMpyftDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGAGKTVA 119
Cdd:cd14937     10 RYKKNYIYTIAEPMLISINPYQVI----DVDINEYKNKNTNELPPHVYSYAKDAMTDFINTKTNQSIIISGESGSGKTEA 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  120 AKYIMGYISKvsgGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNFLLEKSRVVM 199
Cdd:cd14937     86 SKLVIKYYLS---GVKEDNEISNTLWDSNFILEAFGNAKTLKNNNSSRYGKYIKIELDEYQNIVSSSIEIFLLENIRVVS 162
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  200 QNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTyQVDGTDDRSDFGETLSAMQVIGIPPSIQQLVLQLvAG 279
Cdd:cd14937    163 QEEEERGYHIFYQIFNGMSQELKNKYKIRSENEYKYIVNKNV-VIPEIDDAKDFGNLMISFDKMNMHDMKDDLFLTL-SG 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  280 ILHLGNISF--CEDGNYARVESVD-----LLAFPAYLLGIDSGRLQEKL--TSRKMdsrwggRSESIDVTLNVEQAAYTR 350
Cdd:cd14937    241 LLLLGNVEYqeIEKGGKTNCSELDknnleLVNEISNLLGINYENLKDCLvfTEKTI------ANQKIEIPLSVEESVSIC 314
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  351 DALAKGLYARLFDFLVEAINRAMQKPQE-EYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQE 429
Cdd:cd14937    315 KSISKDLYNKIFSYITKRINNFLNNNKElNNYIGILDIFGFEIFSKNSLEQLLINIANEEIHSIYLYIVYEKETELYKAE 394
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  430 GIRWTPIQYFNNKVVCDLIENKLSppgIMSVLDDVCatmhATGGGADQTLLQKLQAAVGTHEHFNS----WSAGFVIHHY 505
Cdd:cd14937    395 DILIESVKYTTNESIIDLLRGKTS---IISILEDSC----LGPVKNDESIVSVYTNKFSKHEKYAStkkdINKNFVIKHT 467
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  506 AGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKKGRPSTAGSKIKKQANDLVATLMRCTPHYIRCI 585
Cdd:cd14937    468 VSDVTYTITNFISKNKDILPSNIVRLLKVSNNKLVRSLYEDVEVSESLGRKNLITFKYLKNLNNIISYLKSTNIYFIKCI 547
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  586 KPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAgFAYRRQFAKFLQRYAILTPETWPRWRGDERQGVQHLLRAvNMEPD 665
Cdd:cd14937    548 KPNENKEKNNFNQKKVFPQLFSLSIIETLNISFF-FQYKYTFDVFLSYFEYLDYSTSKDSSLTDKEKVSMILQN-TVDPD 625
                          650
                   ....*....|..
gi 1622892340  666 QYQMGSTKVFVK 677
Cdd:cd14937    626 LYKVGKTMVFLK 637
MYSc_Myo38 cd14899
class XXXVIII myosin; The class XXXVIII myosins are comprised of Stramenopiles. Not much is ...
32-634 1.25e-104

class XXXVIII myosin; The class XXXVIII myosins are comprised of Stramenopiles. Not much is known about this myosin class. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276864 [Multi-domain]  Cd Length: 717  Bit Score: 345.54  E-value: 1.25e-104
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIdlYQGAAQYENP-------------PHIYALTDNMYRNML 98
Cdd:cd14899      2 SILNALRLRYERHAIYTHIGDILISINPFQDLPQLYGDEI--LRGYAYDHNSqfgdrvtstdprePHLFAVARAAYIDIV 79
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   99 IDCENQCVIISGESGAGKTVAAKYIMGYISKVSGGGNKVQH---------------VKDIILQSNPLLEAFGNAKTVRNN 163
Cdd:cd14899     80 QNGRSQSILISGESGAGKTEATKIIMTYFAVHCGTGNNNLTnsesisppaspsrttIEEQVLQSNPILEAFGNARTVRND 159
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  164 NSSRFGKYFEIQF-SRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEG----ASQEQRQNLGLMT-PDYYYYLN 237
Cdd:cd14899    160 NSSRFGKFIELRFrDERRRLAGARIRTYLLEKIRVIKQAPHERNFHIFYELLSAdnncVSKEQKQVLALSGgPQSFRLLN 239
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  238 QS-DTYQVDGTDDRSDFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISF------CEDGNY---ARVES-----VDL 302
Cdd:cd14899    240 QSlCSKRRDGVKDGVQFRATKRAMQQLGMSEGEIGGVLEIVAAVLHMGNVDFeqiphkGDDTVFadeARVMSsttgaFDH 319
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  303 LAFPAYLLGIDSGRLQEKLTSRKMDSRwggrSESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKP------ 376
Cdd:cd14899    320 FTKAAELLGVSTEALDHALTKRWLHAS----NETLVVGVDVAHARNTRNALTMECYRLLFEWLVARVNNKLQRQasapwg 395
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  377 -------QEEYS---IGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCD 446
Cdd:cd14899    396 adesdvdDEEDAtdfIGLLDIFGFEDMAENSFEQLCINYANEALQHQFNQYIFEEEQRLYRDEGIRWSFVDFPNNRACLE 475
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  447 LIENKlsPPGIMSVLDDVCATMHatggGADQTLLQKLQAAV---GTHEHFNSWSA-----GFVIHHYAGKVSYDVSGFCE 518
Cdd:cd14899    476 LFEHR--PIGIFSLTDQECVFPQ----GTDRALVAKYYLEFekkNSHPHFRSAPLiqrttQFVVAHYAGCVTYTIDGFLA 549
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  519 RNRDVLFSDLIELMQTSEQAFLRMLFPEKLDGDKKGRPS-------------------TAGSKIKKQANDLVATLMRCTP 579
Cdd:cd14899    550 KNKDSFCESAAQLLAGSSNPLIQALAAGSNDEDANGDSEldgfggrtrrraksaiaavSVGTQFKIQLNELLSTVRATTP 629
                          650       660       670       680       690
                   ....*....|....*....|....*....|....*....|....*....|....*
gi 1622892340  580 HYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRY 634
Cdd:cd14899    630 RYVRCIKPNDSHVGSLFQSTRVVEQLRSGGVLEAVRVARAGFPVRLTHKQFLGRY 684
MYSc_Myo37 cd14898
class XXXVII myosin, motor domain; The class XXXVIII myosins are comprised of fungi. Not much ...
31-639 6.73e-97

class XXXVII myosin, motor domain; The class XXXVIII myosins are comprised of fungi. Not much is known about this myosin class. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276863  Cd Length: 578  Bit Score: 320.31  E-value: 6.73e-97
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   31 DAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMpYFTDReIDLYQGAAQYENPpHIYALTDNMYRNMLIDcENQCVIISG 110
Cdd:cd14898      1 NATLEILEKRYASGKIYTKSGLVFLALNPYETI-YGAGA-MKAYLKNYSHVEP-HVYDVAEASVQDLLVH-GNQTIVISG 76
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  111 ESGAGKTVAAKYIMGYISKVSGGGNKVQHvkdIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSrgGEPDGGKISNF 190
Cdd:cd14898     77 ESGSGKTENAKLVIKYLVERTASTTSIEK---LITAANLILEAFGNAKTQLNDNSSRFGKRIKLKFD--GKITGAKFETY 151
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  191 LLEKSRVVMQNENERNFHIYYQLLegASQEQRqnlglMTPDYYYYlnQSDTYQVDGTDDRSDFGETL-SAMQVIGIP--P 267
Cdd:cd14898    152 LLEKSRVTHHEKGERNFHIFYQFC--ASKRLN-----IKNDFIDT--SSTAGNKESIVQLSEKYKMTcSAMKSLGIAnfK 222
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  268 SIQQLVLqlvaGILHLGNISFCEDGNYARVESVDLLAFpAYLLGIDSGRLQEKLTSRKMDSRwggrSESIDVTLNVEQAA 347
Cdd:cd14898    223 SIEDCLL----GILYLGSIQFVNDGILKLQRNESFTEF-CKLHNIQEEDFEESLVKFSIQVK----GETIEVFNTLKQAR 293
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  348 YTRDALAKGLYARLFDFLVEAINRAMQKpQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYV 427
Cdd:cd14898    294 TIRNSMARLLYSNVFNYITASINNCLEG-SGERSISVLDIFGFEIFESNGLDQLCINWTNEKIQNDFIKKMFRAKQGMYK 372
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  428 QEGIRWTPIQYFNNKVVCDLIENklsPPGIMsvldDVCATMHATGGGADQTLLQKLQAAVgthEHFNSWSAG--FVIHHY 505
Cdd:cd14898    373 EEGIEWPDVEFFDNNQCIRDFEK---PCGLM----DLISEESFNAWGNVKNLLVKIKKYL---NGFINTKARdkIKVSHY 442
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  506 AGKVSYDVSGFCERNRD----VLFSDLIELMQTSEQAFLRMLfpekldgdkkgrpstagskiKKQANDLVATLMRCTPHY 581
Cdd:cd14898    443 AGDVEYDLRDFLDKNREkgqlLIFKNLLINDEGSKEDLVKYF--------------------KDSMNKLLNSINETQAKY 502
                          570       580       590       600       610
                   ....*....|....*....|....*....|....*....|....*....|....*...
gi 1622892340  582 IRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTP 639
Cdd:cd14898    503 IKCIRPNEECRPWCFDRDLVSKQLAECGILETIRLSKQCFPQEIPKDRFEERYRILGI 560
MYSc_Myo44 cd14905
class XLIV myosin, motor domain; There is little known about the function of the myosin XLIV ...
31-677 5.07e-95

class XLIV myosin, motor domain; There is little known about the function of the myosin XLIV class. Members here include cellular slime mold Polysphondylium and soil-living amoeba Dictyostelium. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276870  Cd Length: 673  Bit Score: 318.19  E-value: 5.07e-95
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   31 DAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREidLYQGAAQYEN-PPHIYALTDNMYRNMLIDCENQCVIIS 109
Cdd:cd14905      1 DTLINIIQARYKKEIIYTYIGPILVSVNPLRYLPFLHSQE--LVRNYNQRRGlPPHLFALAAKAISDMQDFRRDQLIFIG 78
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  110 GESGAGKTVAAKYIMGYIskVSGGGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISN 189
Cdd:cd14905     79 GESGSGKSENTKIIIQYL--LTTDLSRSKYLRDYILESGIILESFGHASTDSNHNSSRWGKYFEMFYSLYGEIQGAKLYS 156
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  190 FLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQVDGTDDRSDFGETLSAMQVIGIPPSI 269
Cdd:cd14905    157 YFLDENRVTYQNKGERNFHIFYQFLKGITDEEKAAYQLGDINSYHYLNQGGSISVESIDDNRVFDRLKMSFVFFDFPSEK 236
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  270 QQLVLQLVAGILHLGNISFCEDGNYARVESVDLLAFPAYLLGIDSGRLQEKLTSrkmdsrwggrsesiDVTLNVEQAAYT 349
Cdd:cd14905    237 IDLIFKTLSFIIILGNVTFFQKNGKTEVKDRTLIESLSHNITFDSTKLENILIS--------------DRSMPVNEAVEN 302
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  350 RDALAKGLYARLFDFLVEAINRAMQKPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQE 429
Cdd:cd14905    303 RDSLARSLYSALFHWIIDFLNSKLKPTQYSHTLGILDLFGQESSQLNGYEQFSINFLEERLQQIYLQTVLKQEQREYQTE 382
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  430 GIRW-TPIQYFNNKVVCDLIENklsppgIMSVLDDVCATMHATgggaDQTLLQKLQAAVGTHEHFNSWSAGFVIHHYAGK 508
Cdd:cd14905    383 RIPWmTPISFKDNEESVEMMEK------IINLLDQESKNINSS----DQIFLEKLQNFLSRHHLFGKKPNKFGIEHYFGQ 452
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  509 VSYDVSGFCERNRD----------------VLFS------------------DLIELMQTSEQAFLRMLF------PEKL 548
Cdd:cd14905    453 FYYDVRGFIIKNRDeilqrtnvlhknsitkYLFSrdgvfninatvaelnqmfDAKNTAKKSPLSIVKVLLscgsnnPNNV 532
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  549 D------------GDKKGRPSTAGSKIKK-QANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIR 615
Cdd:cd14905    533 NnpnnnsggggggGNSGGGSGSGGSTYTTySSTNKAINNSNCDFHFIRCIKPNSKKTHLTFDVKSVNEQIKSLCLLETTR 612
                          650       660       670       680       690       700       710
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  616 VRRAGFAYRRQFAKFLQRYAILTpetwprwrgDERQGVQHLLRA-----VNME---PDQYQMGSTKVFVK 677
Cdd:cd14905    613 IQRFGYTIHYNNKIFFDRFSFFF---------QNQRNFQNLFEKlkendINIDsilPPPIQVGNTKIFLR 673
MYSc_Myo26 cd14887
class XXVI myosin, motor domain; These MyTH-FERM myosins are thought to be related to the ...
35-675 1.11e-93

class XXVI myosin, motor domain; These MyTH-FERM myosins are thought to be related to the other myosins that have a MyTH4 domain such as class III, VII, IX, X , XV, XVI, XVII, XX, XXII, XXV, and XXXIV. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276852  Cd Length: 725  Bit Score: 315.82  E-value: 1.11e-93
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   35 ANLRKRFMDDY--------IFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCV 106
Cdd:cd14887      5 ENLYQRYNKAYinkenrncIYTYTGTLLIAVNPYRFFNLYDRQWISRFDTEANSRLVPHPFGLAEFAYCRLVRDRRSQSI 84
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  107 IISGESGAGKTVAAKYIMGYISKVSG--GGNKVQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDG 184
Cdd:cd14887     85 LISGESGAGKTETSKHVLTYLAAVSDrrHGADSQGLEARLLQSGPVLEAFGNAHTVLNANSSRFGKMLLLHFTGRGKLTR 164
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  185 GKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYlnqsdtyqvdgtddrsDFGETLSAMQVIG 264
Cdd:cd14887    165 ASVATYLLANERVVRIPSDEFSFHIFYALCNAAVAAATQKSSAGEGDPEST----------------DLRRITAAMKTVG 228
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  265 IPPSIQQLVLQLVAGILHLGNISFCEDGN---------------------------YARVESVDL---------LAFPAY 308
Cdd:cd14887    229 IGGGEQADIFKLLAAILHLGNVEFTTDQEpetskkrkltsvsvgceetaadrshssEVKCLSSGLkvteasrkhLKTVAR 308
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  309 LLGIDSGRLQEKLTSRKMDSRwggRSESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQ---KPQEEYS---- 381
Cdd:cd14887    309 LLGLPPGVEGEEMLRLALVSR---SVRETRSFFDLDGAAAARDAACKNLYSRAFDAVVARINAGLQrsaKPSESDSdedt 385
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  382 --------IGVLDIYGFEIFQ---KNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIEN 450
Cdd:cd14887    386 psttgtqtIGILDLFGFEDLRnhsKNRLEQLCINYANERLHCFLLEQLILNEHMLYTQEGVFQNQDCSAFPFSFPLASTL 465
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  451 KLSP------------------------PGIMSVLDDVCATMHATGGGADQTLL---QKLQAAVGTHEHFNSWSA----- 498
Cdd:cd14887    466 TSSPsstspfsptpsfrsssafatspslPSSLSSLSSSLSSSPPVWEGRDNSDLfyeKLNKNIINSAKYKNITPAlsren 545
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  499 -GFVIHHYAGKVSYDVSGFCERNRDVLfSDLIELMQTSEQAFLRMLFPEKLDGDK--KGRPSTAGSKIKKQANDLVATLM 575
Cdd:cd14887    546 lEFTVSHFACDVTYDARDFCRANREAT-SDELERLFLACSTYTRLVGSKKNSGVRaiSSRRSTLSAQFASQLQQVLKALQ 624
                          650       660       670       680       690       700       710       720
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  576 RCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWRgDERQGVQH 655
Cdd:cd14887    625 ETSCHFIRCVKPNRVQEAGIFEDAYVHRQLRCSGMSDLLRVMADGFPCRLPYVELWRRYETKLPMALREAL-TPKMFCKI 703
                          730       740
                   ....*....|....*....|
gi 1622892340  656 LLRAVNMEPDQYQMGSTKVF 675
Cdd:cd14887    704 VLMFLEINSNSYTFGKTKIF 723
MYSc_Myo23 cd14884
class XXIII myosin, motor domain; These myosins are predicted to have a neck region with 1-2 ...
33-624 2.58e-91

class XXIII myosin, motor domain; These myosins are predicted to have a neck region with 1-2 IQ motifs and a single MyTH4 domain in its C-terminal tail. The lack of a FERM domain here is odd since MyTH4 domains are usually found alongside FERM domains where they bind to microtubules. At any rate these Class XXIII myosins are still proposed to function in the apicomplexan microtubule cytoskeleton. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276850 [Multi-domain]  Cd Length: 685  Bit Score: 307.99  E-value: 2.58e-91
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   33 IAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDRE-IDLY-----QGAAQYEN--PPHIYALTDNMYRNMLIDCENQ 104
Cdd:cd14884      3 VLQNLKNRYLKNKIYTFHASLLLALNPYKPLKELYDQDvMNVYlhkksNSAASAAPfpKAHIYDIANMAYKNMRGKLKRQ 82
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  105 CVIISGESGAGKTVAAKYIMGYISKVSGGGNKVQHVkDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQF-SRGGEPD 183
Cdd:cd14884     83 TIVVSGHSGSGKTENCKFLFKYFHYIQTDSQMTERI-DKLIYINNILESMSNATTIKNNNSSRCGRINLLIFeEVENTQK 161
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  184 --------GGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQ--RQNL-------GLMTPDYYYYLNQS------- 239
Cdd:cd14884    162 nmfngcfrNIKIKILLLEINRCIAHNFGERNFHVFYQVLRGLSDEDlaRRNLvrncgvyGLLNPDESHQKRSVkgtlrlg 241
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  240 ----DTYQVDGTDDRSDFGETLSAMQVIGIPPSIQQLVLQLVAGILHLGNisfcedgnyarvesvDLLAFPAYLLGIDSG 315
Cdd:cd14884    242 sdslDPSEEEKAKDEKNFVALLHGLHYIKYDERQINEFFDIIAGILHLGN---------------RAYKAAAECLQIEEE 306
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  316 RLQEKLTSRKMDSRwggrSESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS-------------I 382
Cdd:cd14884    307 DLENVIKYKNIRVS----HEVIRTERRKENATSTRDTLIKFIYKKLFNKIIEDINRNVLKCKEKDEsdnediysineaiI 382
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  383 GVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQEGIRWtpiqyfNNKVVCDLIENKLSPPGIMSVLD 462
Cdd:cd14884    383 SILDIYGFEELSGNDFDQLCINLANEKLNNYYINNEIEKEKRIYARENIIC------CSDVAPSYSDTLIFIAKIFRRLD 456
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  463 DVcATMHATG-------------GGADQTLLQKLQAAVGTHEHFNSWSAG--------FVIHHYAGKVSYDVSGFCERNR 521
Cdd:cd14884    457 DI-TKLKNQGqkktddhffryllNNERQQQLEGKVSYGFVLNHDADGTAKkqnikkniFFIRHYAGLVTYRINNWIDKNS 535
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  522 DVLFSDLIELMQTSEQAFLRmlfpEKLDGDKKGRPSTAGSKIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRV 601
Cdd:cd14884    536 DKIETSIETLISCSSNRFLR----EANNGGNKGNFLSVSKKYIKELDNLFTQLQSTDMYYIRCFLPNAKMLPNTFKRLLV 611
                          650       660
                   ....*....|....*....|...
gi 1622892340  602 KHQVEYLGLKENIRVRRAGFAYR 624
Cdd:cd14884    612 YRQLKQCGSNEMIKILNRGLSHK 634
MYSc_Myo18 cd01386
class XVIII myosin, motor domain; Many members of this class contain a N-terminal PDZ domain ...
37-677 3.84e-86

class XVIII myosin, motor domain; Many members of this class contain a N-terminal PDZ domain which is commonly found in proteins establishing molecular complexes. The motor domain itself does not exhibit ATPase activity, suggesting that it functions as an actin tether protein. It also has two IQ domains that probably bind light chains or related calmodulins and a C-terminal tail with two sections of coiled-coil domains, which are thought to mediate homodimerization. The function of these myosins are largely unknown. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276837 [Multi-domain]  Cd Length: 689  Bit Score: 293.83  E-value: 3.84e-86
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   37 LRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGAGK 116
Cdd:cd01386      7 LRQRYGANLIHTYAGPSLIVINPRHPLAVYSEKVAKMFKGCRREDMPPHIYASAQSAYRAMLMSRRDQSIVLLGRSGSGK 86
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  117 TVAAKYIMGYISKVSGGGNKVQHVkDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNFLLEKSR 196
Cdd:cd01386     87 TTNCRHILEYLVTAAGSVGGVLSV-EKLNAALTVLEAFGNVRTALNGNATRFSQLFSLDFDQAGQLASASIQTLLLERSR 165
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  197 VVMQNENERNFHIYYQLLEGASQEQRQNLGL--MTPDYYYYLNQSDTyQVDGTDDRSDFGETLSAMQVIGIPPSIQQLVL 274
Cdd:cd01386    166 VARRPEGESNFNVFYYLLAGADAALRTELHLnqLAESNSFGIVPLQK-PEDKQKAAAAFSKLQAAMKTLGISEEEQRAIW 244
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  275 QLVAGILHLGNISFCEDGN-----YARVESVDllaFPAYLLGID-------------SGRLQEKLTSRkmdSRWGGRSES 336
Cdd:cd01386    245 SILAAIYHLGAAGATKAASagrkqFARPEWAQ---RAAYLLGCTleelssaifkhhlSGGPQQSTTSS---GQESPARSS 318
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  337 IDVTLNVEQAAYtrDALAKGLYARLFDFLVEAINRAMQKPQEE-YSIGVLDIYGFEI--FQKN----GFEQFCINFVNEK 409
Cdd:cd01386    319 SGGPKLTGVEAL--EGFAAGLYSELFAAVVSLINRSLSSSHHStSSITIVDTPGFQNpaHSGSqrgaTFEDLCHNYAQER 396
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  410 LQQIFIELTLKAEQEEYVQEGIrwtPIQYfnnkvvcDLIEnkLSPPGIMSVLDDVC---------ATMHATG-------- 472
Cdd:cd01386    397 LQLLFHERTFVAPLERYKQENV---EVDF-------DLPE--LSPGALVALIDQAPqqalvrsdlRDEDRRGllwlldee 464
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  473 ----GGADQTLLQKLQAAVGTHEHFNSWSA--------GFVIHHYAGK--VSYDVSGFCERNR-DVLFSDLIELMQTSEQ 537
Cdd:cd01386    465 alypGSSDDTFLERLFSHYGDKEGGKGHSLlrrsegplQFVLGHLLGTnpVEYDVSGWLKAAKeNPSAQNATQLLQESQK 544
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  538 aflrmlfpeKLDGDKKGRPStagSKIKKQANDLVATLMRCTPHYIRCIKPN------ETKRPRDWEENR------VKHQV 605
Cdd:cd01386    545 ---------ETAAVKRKSPC---LQIKFQVDALIDTLRRTGLHFVHCLLPQhnagkdERSTSSPAAGDElldvplLRSQL 612
                          650       660       670       680       690       700       710
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1622892340  606 EYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPE-----TWPRWRGDERQGVQHLLRAVNMEPDQYQMGSTKVFVK 677
Cdd:cd01386    613 RGSQLLDALRLYRQGFPDHMPLGEFRRRFQVLAPPltkklGLNSEVADERKAVEELLEELDLEKSSYRIGLSQVFFR 689
MYSc_Myo20 cd14881
class XX myosin, motor domain; These class 20 myosins are primarily insect myosins with such ...
31-651 2.39e-80

class XX myosin, motor domain; These class 20 myosins are primarily insect myosins with such members as Drosophila, Daphnia, and mosquitoes. These myosins contain a single IQ motif in the neck region. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276847 [Multi-domain]  Cd Length: 633  Bit Score: 276.22  E-value: 2.39e-80
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   31 DAIAANLRKRFMDDYIFTYIGSVLISVNPFkqmpyfTDREIDLYQGAAQYENP-PHIYALTDNMYRNMLIDCENQCVIIS 109
Cdd:cd14881      1 DAVMKCLQARFYAKEFFTNVGPILLSVNPY------RDVGNPLTLTSTRSSPLaPQLLKVVQEAVRQQSETGYPQAIILS 74
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  110 GESGAGKTVAAKYIMGYISKVSGGGNKVQHVKDIIlQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSrggepDG----G 185
Cdd:cd14881     75 GTSGSGKTYASMLLLRQLFDVAGGGPETDAFKHLA-AAFTVLRSLGSAKTATNSESSRIGHFIEVQVT-----DGalyrT 148
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  186 KISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGL--MTPDYYYYLNQSDTYQvDGTDDRSDFGETLSAMQVI 263
Cdd:cd14881    149 KIHCYFLDQTRVIRPLPGEKNYHIFYQMLAGLSQEERVKLHLdgYSPANLRYLSHGDTRQ-NEAEDAARFQAWKACLGIL 227
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  264 GIPPSIqqlVLQLVAGILHLGNISFCE-DGNYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSRwGGRSESIDvtlN 342
Cdd:cd14881    228 GIPFLD---VVRVLAAVLLLGNVQFIDgGGLEVDVKGETELKSVAALLGVSGAALFRGLTTRTHNAR-GQLVKSVC---D 300
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  343 VEQAAYTRDALAKGLYARLFDFLVEAINR------AMQKPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIE 416
Cdd:cd14881    301 ANMSNMTRDALAKALYCRTVATIVRRANSlkrlgsTLGTHATDGFIGILDMFGFEDPKPSQLEHLCINLCAETMQHFYNT 380
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  417 LTLKAEQEEYVQEGIRW-TPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMhatggGADQTLLQKLQAAvgtHEHfNS 495
Cdd:cd14881    381 HIFKSSIESCRDEGIQCeVEVDYVDNVPCIDLISSL--RTGLLSMLDVECSPR-----GTAESYVAKIKVQ---HRQ-NP 449
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  496 WSAG--------FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELM--QTSEQAFLRML--FPEKLDgdkkgrpstagski 563
Cdd:cd14881    450 RLFEakpqddrmFGIRHFAGRVVYDASDFLDTNRDVVPDDLVAVFykQNCNFGFATHTqdFHTRLD-------------- 515
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  564 kkqanDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWP 643
Cdd:cd14881    516 -----NLLRTLVHARPHFVRCIRSNTTETPNHFDRGTVVRQIRSLQVLETVNLMAGGYPHRMRFKAFNARYRLLAPFRLL 590

                   ....*...
gi 1622892340  644 RwRGDERQ 651
Cdd:cd14881    591 R-RVEEKA 597
MYSc_Myo21 cd14882
class XXI myosin, motor domain; The myosins here are comprised of insects. Leishmania class ...
31-677 5.18e-79

class XXI myosin, motor domain; The myosins here are comprised of insects. Leishmania class XXI myosins do not group with them. Myo21, unlike other myosin proteins, contains UBA-like protein domains and has no structural or functional relationship with the myosins present in other organisms possessing cilia or flagella. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. They have diverse tails with IQ, WW, PX, and Tub domains. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276848  Cd Length: 642  Bit Score: 272.77  E-value: 5.18e-79
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   31 DAIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISG 110
Cdd:cd14882      1 ENILEELRHRYLMGESYTFIGDILLSLNPNEIKQEYPQEFHAKYRCKSRSDNAPHIFSVADSAYQDMLHHEEPQHIILSG 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  111 ESGAGKTVAAKYIMGYISkVSGGGNkvQHVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNF 190
Cdd:cd14882     81 ESYSGKTTNARLLIKHLC-YLGDGN--RGATGRVESSIKAILALVNAGTPLNADSTRCILQYQLTFGSTGKMSGAIFWMY 157
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  191 LLEKSRVVMQNENERNFHIYYQLLEGASQEQR-QNLGLMTPDYYYYLNQSDTYQVDGTDDRSD--------FGETLSAMQ 261
Cdd:cd14882    158 QLEKLRVSTTDGNQSNFHIFYYFYDFIEAQNRlKEYNLKAGRNYRYLRIPPEVPPSKLKYRRDdpegnverYKEFEEILK 237
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  262 VIGIPPSIQQLVLQLVAGILHLGNISFCEDGNYARVESVDLLAFPAYLLGIDSGRLQEKLTSRKMDSRwgGRSESIDVTl 341
Cdd:cd14882    238 DLDFNEEQLETVRKVLAAILNLGEIRFRQNGGYAELENTEIASRVAELLRLDEKKFMWALTNYCLIKG--GSAERRKHT- 314
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  342 nVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQ----EEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIEL 417
Cdd:cd14882    315 -TEEARDARDVLASTLYSRLVDWIINRINMKMSFPRavfgDKYSISIHDMFGFECFHRNRLEQLMVNTLNEQMQYHYNQR 393
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  418 TLKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENKlsPPGIMSVLDDVCATMHATgggadQTLLQKLQAAVGTHEHFNSwS 497
Cdd:cd14882    394 IFISEMLEMEEEDIPTINLRFYDNKTAVDQLMTK--PDGLFYIIDDASRSCQDQ-----NYIMDRIKEKHSQFVKKHS-A 465
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  498 AGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFpeklDGDKKGRPSTAGSKIKKQANDLVATLMRC 577
Cdd:cd14882    466 HEFSVAHYTGRIIYDAREFADKNRDFVPPEMIETMRSSLDESVKLMF----TNSQVRNMRTLAATFRATSLELLKMLSIG 541
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  578 T----PHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETwprwrgDE---- 649
Cdd:cd14882    542 AnsggTHFVRCIRSDLEYKPRGFHSEVVRQQMRALAVLDTAKARQKGFSYRIPFQEFLRRYQFLAFDF------DEtvem 615
                          650       660
                   ....*....|....*....|....*....
gi 1622892340  650 -RQGVQHLLRAVNMEpdQYQMGSTKVFVK 677
Cdd:cd14882    616 tKDNCRLLLIRLKME--GWAIGKTKVFLK 642
MYSc_Myo12 cd14874
class XXXIII myosin, motor domain; Little is known about the XXXIII class of myosins. They ...
32-677 2.97e-77

class XXXIII myosin, motor domain; Little is known about the XXXIII class of myosins. They are found predominately in nematodes. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276841 [Multi-domain]  Cd Length: 628  Bit Score: 267.51  E-value: 2.97e-77
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   32 AIAANLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYqgaaqyenppHIYALTDNMYRNMLIDCEN-QCVIISG 110
Cdd:cd14874      2 GIAQNLHERFKKGQTYTKASNVLVFVNDFNKLSIQDQLVIKKC----------HISGVAENALDRIKSMSSNaESIVFGG 71
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  111 ESGAGKTVAAKYIMGYISKVSGGGNKVQHVKDIilqsNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEPDGGKISNF 190
Cdd:cd14874     72 ESGSGKSYNAFQVFKYLTSQPKSKVTTKHSSAI----ESVFKSFGCAKTLKNDEATRFGCSIDLLYKRNVLTGLNLKYTV 147
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  191 LLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLNQSDTYQvDGTDDRSDFGETLSAMQVIGIPPSIQ 270
Cdd:cd14874    148 PLEVPRVISQKPGERNFNVFYEVYHGLNDEMKAKFGIKGLQKFFYINQGNSTE-NIQSDVNHFKHLEDALHVLGFSDDHC 226
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  271 QLVLQLVAGILHLGNISF------------CEDGNYARVESVdllafpAYLLGIDSGRLQEKLTSRKMDSrwggrsesid 338
Cdd:cd14874    227 ISIYKIISTILHIGNIYFrtkrnpnveqdvVEIGNMSEVKWV------AFLLEVDFDQLVNFLLPKSEDG---------- 290
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  339 VTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELT 418
Cdd:cd14874    291 TTIDLNAALDNRDSFAMLIYEELFKWVLNRIGLHLKCPLHTGVISILDHYGFEKYNNNGVEEFLINSVNERIENLFVKHS 370
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  419 LKAEQEEYVQEGIR---WTPIQYFNNKVVcDLIENKlsPPGIMSVLDDVCATMHatggGADQTLLQKLQAavgthEHFNS 495
Cdd:cd14874    371 FHDQLVDYAKDGISvdyKVPNSIENGKTV-ELLFKK--PYGLLPLLTDECKFPK----GSHESYLEHCNL-----NHTDR 438
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  496 WSAG---------FVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQAFLRMLFpEKLDGDKKGRPSTAGSKIKKQ 566
Cdd:cd14874    439 SSYGkarnkerleFGVRHCIGTTWYNVTDFFSRNKRIISLSAVQLLRSSKNPIIGLLF-ESYSSNTSDMIVSQAQFILRG 517
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  567 ANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTPETWPRWR 646
Cdd:cd14874    518 AQEIADKINGSHAHFVRCIKSNNERQPKKFDIPLVNRQIKNLLLAELLSFRIKGYPVKISKTTFARQYRCLLPGDIAMCQ 597
                          650       660       670
                   ....*....|....*....|....*....|...
gi 1622892340  647 gDERQGVQHLL--RAVNMEPDqYQMGSTKVFVK 677
Cdd:cd14874    598 -NEKEIIQDILqgQGVKYEND-FKIGTEYVFLR 628
MYSc_Myo32 cd14893
class XXXII myosin, motor domain; Class XXXII myosins do not contain any IQ motifs, but ...
37-676 1.70e-74

class XXXII myosin, motor domain; Class XXXII myosins do not contain any IQ motifs, but possess tandem MyTH4 and FERM domains. The myosin classes XXX to XXXIV contain members from Phytophthora species and Hyaloperonospora parasitica. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276858  Cd Length: 741  Bit Score: 262.60  E-value: 1.70e-74
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   37 LRKRFMDDYIFTYIGSVLISVNPFKQMPYFT----------DREIDLYQGAAQYENPPHIYALTDNMYRNMLIDCENQCV 106
Cdd:cd14893      7 LRARYRMEQVYTWVDRVLVGVNPVTPLPIYTpdhmqaynksREQTPLYEKDTVNDAPPHVFALAQNALRCMQDAGEDQAV 86
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  107 IISGESGAGKTVAAKYIMGYISKV---------SGGGNKVQH-VKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQF 176
Cdd:cd14893     87 ILLGGMGAGKSEAAKLIVQYLCEIgdeteprpdSEGASGVLHpIGQQILHAFTILEAFGNAATRQNRNSSRFAKMISVEF 166
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  177 SRGGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQ--RQNLGL-MTPDYYYYLNQSDTYQVDGTDDRSDF 253
Cdd:cd14893    167 SKHGHVIGGGFTTHYFEKSRVIDCRSHERNFHVFYQVLAGVQHDPtlRDSLEMnKCVNEFVMLKQADPLATNFALDARDY 246
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  254 GETLSAMQVIGIPPSIQQLVLQLVAGILHLGNISFCEDG------NYARVESVD-------------LLAfpAYLLGIDS 314
Cdd:cd14893    247 RDLMSSFSALRIRKNQRVEIVRIVAALLHLGNVDFVPDPeggksvGGANSTTVSdaqscalkdpaqiLLA--AKLLEVEP 324
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  315 GRLQEKLTSRKMDSRWGGRSESIDVTLNVEQAAYTRDALAKGLYARLFDFLVEAINRAMQKPQEEYS----------IGV 384
Cdd:cd14893    325 VVLDNYFRTRQFFSKDGNKTVSSLKVVTVHQARKARDTFVRSLYESLFNFLVETLNGILGGIFDRYEksnivinsqgVHV 404
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  385 LDIYGFEIF--QKNGFEQFCINFVNEKLQQIFIELTLK-----AEQEEYVQEGiRWT-----PIQYFNNKVVcDLIENKl 452
Cdd:cd14893    405 LDMVGFENLtpSQNSFDQLCFNYWSEKVHHFYVQNTLAinfsfLEDESQQVEN-RLTvnsnvDITSEQEKCL-QLFEDK- 481
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  453 sPPGIMSVLDDVCATMHATgggaDQTLLQKLQA---AVG--THEHFNS------------WSAGFVIHHYAGKVSYDVSG 515
Cdd:cd14893    482 -PFGIFDLLTENCKVRLPN----DEDFVNKLFSgneAVGglSRPNMGAdttneylapskdWRLLFIVQHHCGKVTYNGKG 556
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  516 FCERNRDVLFSDLIELMQTSEQAFLRMLFPEKL--------------DGDKKG---------RPSTAGSK-----IKKQA 567
Cdd:cd14893    557 LSSKNMLSISSTCAAIMQSSKNAVLHAVGAAQMaaassekaakqteeRGSTSSkfrksassaRESKNITDsaatdVYNQA 636
                          650       660       670       680       690       700       710       720
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  568 NDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTpetwprwrg 647
Cdd:cd14893    637 DALLHALNHTGKNFLVCIKPNETLEEGVFDSAYVMKQIRMNHLVELMQASRSIFTVHLTYGHFFRRYKNVC--------- 707
                          730       740       750
                   ....*....|....*....|....*....|...
gi 1622892340  648 DERQGVQHLLRAVN----MEPDQYQMGSTKVFV 676
Cdd:cd14893    708 GHRGTLESLLRSLSaigvLEEEKFVVGKTKVYL 740
Myosin_TH1 pfam06017
Unconventional myosin tail, actin- and lipid-binding; Unconventional myosins, ie those that ...
750-946 2.13e-61

Unconventional myosin tail, actin- and lipid-binding; Unconventional myosins, ie those that are not found in muscle, have the common, classical-type head domain, sometimes a neck with the IQ calmodulin-binding motifs, and then non-standard tails. These tails determine the subcellular localization of the unconventional myosins and also help determine their individual functions. The family carries several different unconventional myosins, eg. Myo1f is expressed mainly in immune cells as well as in the inner ear where it can be associated with deafness, Myo1d has a lipid-binding module in their tail and is implicated in endosome vesicle recycling in epithelial cells. Myo1a, b, c and g from various eukaryotes are also found in this family.


Pssm-ID: 461801  Cd Length: 196  Bit Score: 207.84  E-value: 2.13e-61
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  750 AASNILLNKKERRRNSINRNFVGDYLGLEER-----PELRQFLGK--RERVDFADSVTKYDRRFKPIKRDLILTPKCVYV 822
Cdd:pfam06017    3 YASDLLKGRKERRRFSLLRRFMGDYLGLENNfsgpgPKLRKAVGIggDEKVLFSDRVSKFNRSSKPSPRILILTDKAVYL 82
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  823 IGREKVKKGpekgqVREVLKKKLDIQALRGVSLSTRQDDFFILQEDAV---DSFLESVFKTEFVSLLCKRFEEATRRPLP 899
Cdd:pfam06017   83 IDQKKLKNG-----LQYVLKRRIPLSDITGVSVSPLQDDWVVLHLGSPqkgDLLLECDFKTELVTHLSKAYKKKTNRKLN 157
                          170       180       190       200
                   ....*....|....*....|....*....|....*....|....*..
gi 1622892340  900 LTFSDTLQFRVKKegwggGGTRSVTFSRGSGDlavLKVGGRTLTVSV 946
Cdd:pfam06017  158 VKIGDTIEYRKKK-----GKIRTVKFVKDEPK---GKDSYKSGTVSV 196
MYSc_Myo24B cd14938
class XXIV B myosin, motor domain; These myosins have a 1-2 IQ motifs in their neck and a ...
36-676 2.90e-45

class XXIV B myosin, motor domain; These myosins have a 1-2 IQ motifs in their neck and a coiled-coil region in their C-terminal tail. The functions of these myosins remain elusive. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276898 [Multi-domain]  Cd Length: 713  Bit Score: 175.41  E-value: 2.90e-45
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   36 NLRKRFMDDYIFTYIGSVLISVNPFKQMPYFTDREIDLYQGAAQYENPP-HIYALTDNMYRNMLIDCENQCVIISGESGA 114
Cdd:cd14938      6 HLKERFKNNKFYTKMGPLLIFINPKINNNINNEETIEKYKCIDCIEDLSlNEYHVVHNALKNLNELKRNQSIIISGESGS 85
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  115 GKTVAAKYIMGYIS-------KVSGGGNKVQHVKD--------------IILQSNPLLEAFGNAKTVRNNNSSRFGKYFE 173
Cdd:cd14938     86 GKSEIAKNIINFIAyqvkgsrRLPTNLNDQEEDNIhneentdyqfnmseMLKHVNVVMEAFGNAKTVKNNNSSRFSKFCT 165
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  174 IQFSRgGEPDGGKISNFLLEKSRVVMQNENERNFHIYYQLLEGASQEQRQNLGLMTPDYYYYLN---------------- 237
Cdd:cd14938    166 IHIEN-EEIKSFHIKKFLLDKERLINRKANENSFNIFYYIINGSSDKFKKMYFLKNIENYSMLNnekgfekfsdysgkil 244
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  238 ---QSDTYQVDgTDDRSDFGET-LSAM------QVIGIPPSIQQLVLQLVAGI-----LHLGNISFCEDGNYARVESVDL 302
Cdd:cd14938    245 ellKSLNYIFD-DDKEIDFIFSvLSALlllgntEIVKAFRKKSLLMGKNQCGQninyeTILSELENSEDIGLDENVKNLL 323
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  303 LAfpAYLLGIDSGRLQEKLTSRKMdsrwggRSESIDVTLNVEQAAYTR-DALAKGLYARLFDFLVEAINR---AMQK-PQ 377
Cdd:cd14938    324 LA--CKLLSFDIETFVKYFTTNYI------FNDSILIKVHNETKIQKKlENFIKTCYEELFNWIIYKINEkctQLQNiNI 395
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  378 EEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQIFIELTLKAEQEEYVQEGIRWT-PIQYFNNKVVCDLIENKlSPPG 456
Cdd:cd14938    396 NTNYINVLDMAYFENSKDNSLEQLLINTTNEEIIKIKNDCLYKKRVLSYNEDGIFCEyNSENIDNEPLYNLLVGP-TEGS 474
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  457 IMSVLDDVCATMHATGGGADQTLLQKL--QAAVGTHEHFNSWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQT 534
Cdd:cd14938    475 LFSLLENVSTKTIFDKSNLHSSIIRKFsrNSKYIKKDDITGNKKTFVITHSCGDIIYNAENFVEKNIDILTNRFIDMVKQ 554
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  535 SEQAFLR---MLFPEKLDG---DKKGRPS--TAGSKIKKQ---ANDLVATLMR--------------CtpHYIRCIKPNE 589
Cdd:cd14938    555 SENEYMRqfcMFYNYDNSGnivEEKRRYSiqSALKLFKRRydtKNQMAVSLLRnnlteleklqettfC--HFIVCMKPNE 632
                          650       660       670       680       690       700       710       720
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  590 TKRP-RDWEENRVKHQVEYLGLKENIRVRRAGFAYRRQFAKFLQRYAILTpetwprwrGDERQGVQHLLRAVNMEPDQYQ 668
Cdd:cd14938    633 SKRElCSFDANIVLRQVRNFSIVEASQLKVGYYPHKFTLNEFLSIFDIKN--------EDLKEKVEALIKSYQISNYEWM 704

                   ....*...
gi 1622892340  669 MGSTKVFV 676
Cdd:cd14938    705 IGNNMIFL 712
Motor_domain cd01363
Myosin and Kinesin motor domain; Myosin and Kinesin motor domain. These ATPases belong to the ...
53-174 6.67e-43

Myosin and Kinesin motor domain; Myosin and Kinesin motor domain. These ATPases belong to the P-loop NTPase family and provide the driving force in myosin and kinesin mediated processes. Some of the names do not match with what is given in the sequence list. This is because they are based on the current nomenclature by Kollmar/Sebe-Pedros.


Pssm-ID: 276814 [Multi-domain]  Cd Length: 170  Bit Score: 154.04  E-value: 6.67e-43
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340   53 VLISVNPFKQMPYFTDREIDL-YQGAAQYENPPHIYALTDNMYRNMLIDCENQCVIISGESGAGKTVAAKYIMGYISKVS 131
Cdd:cd01363      1 VLVRVNPFKELPIYRDSKIIVfYRGFRRSESQPHVFAIADPAYQSMLDGYNNQSIFAYGESGAGKTETMKGVIPYLASVA 80
                           90       100       110       120       130
                   ....*....|....*....|....*....|....*....|....*....|....*.
gi 1622892340  132 G---GGNKVQ----------HVKDIILQSNPLLEAFGNAKTVRNNNSSRFGKYFEI 174
Cdd:cd01363     81 FngiNKGETEgwvylteitvTLEDQILQANPILEAFGNAKTTRNENSSRFGKFIEI 136
MYSc_Myo33 cd14894
class myosin, motor domain; Class XXXIII myosins have variable numbers of IQ domain and 2 ...
143-642 4.21e-33

class myosin, motor domain; Class XXXIII myosins have variable numbers of IQ domain and 2 tandem ANK repeats that are separated by a PH domain. The myosin classes XXX to XXXIV contain members from Phytophthora species and Hyaloperonospora parasitica. The catalytic (head) domain has ATPase activity and belongs to the larger group of P-loop NTPases. Myosins are actin-dependent molecular motors that play important roles in muscle contraction, cell motility, and organelle transport. The head domain is a molecular motor, which utilizes ATP hydrolysis to generate directed movement toward the plus end along actin filaments. A cyclical interaction between myosin and actin provides the driving force. Rates of ATP hydrolysis and consequently the speed of movement along actin filaments vary widely, from about 0.04 micrometer per second for myosin I to 4.5 micrometer per second for myosin II in skeletal muscle. Myosin II moves in discrete steps about 5-10 nm long and generates 1-5 piconewtons of force. Upon ATP binding, the myosin head dissociates from an actin filament. ATP hydrolysis causes the head to pivot and associate with a new actin subunit. The release of Pi causes the head to pivot and move the filament (power stroke). Release of ADP completes the cycle. CyMoBase classifications were used to confirm and identify the myosins in this hierarchy.


Pssm-ID: 276859 [Multi-domain]  Cd Length: 871  Bit Score: 138.72  E-value: 4.21e-33
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  143 IILQSNPLLEAFGNAKTVRNNNSSRFGKYFEIQFSRGGEP-----DGGKISNFLLEKSRVVMQ------NENERNFHIYY 211
Cdd:cd14894    248 IVLDSNIVLEAFGHATTSMNLNSSRFGKMTTLQVAFGLHPwefqiCGCHISPFLLEKSRVTSErgresgDQNELNFHILY 327
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  212 QLLEGASQ-------EQRQNLGLMTPDYYYYLNQSDtYQVDGTDDRSD--------FGETLSAMQVIGIPPSIQQLVLQL 276
Cdd:cd14894    328 AMVAGVNAfpfmrllAKELHLDGIDCSALTYLGRSD-HKLAGFVSKEDtwkkdverWQQVIDGLDELNVSPDEQKTIFKV 406
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  277 VAGILHLGNIS--FCEDGNYARVESVDLLAFP---AYLLGIDS-GRLQEKLTSRKMDSRwgGRSESIDVTLNVEQAAYTR 350
Cdd:cd14894    407 LSAVLWLGNIEldYREVSGKLVMSSTGALNAPqkvVELLELGSvEKLERMLMTKSVSLQ--STSETFEVTLEKGQVNHVR 484
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  351 DALAKGLYARLFDFLVEAINRAMQ------------------KPQEEYSIGVLDIYGFEIFQKNGFEQFCINFVNEKLQQ 412
Cdd:cd14894    485 DTLARLLYQLAFNYVVFVMNEATKmsalstdgnkhqmdsnasAPEAVSLLKIVDVFGFEDLTHNSLDQLCINYLSEKLYA 564
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  413 ifieltlKAEQEEYVQEGIRWTPIQYFNNKVVCDLIENklsPPGIMSVLDDVCATMHATGGGADQTLLQ----------- 481
Cdd:cd14894    565 -------REEQVIAVAYSSRPHLTARDSEKDVLFIYEH---PLGVFASLEELTILHQSENMNAQQEEKRnklfvrniydr 634
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  482 ---------KLQAAVGTHEHFNSWSAGFVIHHYAGKVSYDVSGFCERNRDVLFSDLIELMQTSEQA-FLRML-------- 543
Cdd:cd14894    635 nssrlpeppRVLSNAKRHTPVLLNVLPFVIPHTRGNVIYDANDFVKKNSDFVYANLLVGLKTSNSShFCRMLnessqlgw 714
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  544 ---FPEKLDGDKKGRPSTAGS---KIKKQANDLVATLMRCTPHYIRCIKPNETKRPRDWEENRVKHQVEYLGLKENIRV- 616
Cdd:cd14894    715 spnTNRSMLGSAESRLSGTKSfvgQFRSHVNVLTSQDDKNMPFYFHCIRPNAKKQPSLVNNDLVEQQCRSQRLIRQMEIc 794
                          570       580
                   ....*....|....*....|....*....
gi 1622892340  617 RRAGFAYRR---QFAKFLQRYAILTPETW 642
Cdd:cd14894    795 RNSSSSYSAidiSKSTLLTRYGSLLREPY 823
SH3_MyoIe_If_like cd11827
Src homology 3 domain of Myosins Ie, If, and similar proteins; Myosins Ie (MyoIe) and If ...
1081-1133 1.71e-30

Src homology 3 domain of Myosins Ie, If, and similar proteins; Myosins Ie (MyoIe) and If (MyoIf) are nonmuscle, unconventional, long tailed, class I myosins containing an N-terminal motor domain and a myosin tail with TH1, TH2, and SH3 domains. MyoIe interacts with the endocytic proteins, dynamin and synaptojanin-1, through its SH3 domain; it may play a role in clathrin-dependent endocytosis. In the kidney, MyoIe is critical for podocyte function and normal glomerular filtration. Mutations in MyoIe is associated with focal segmental glomerulosclerosis, a disease characterized by massive proteinuria and progression to end-stage kidney disease. MyoIf is predominantly expressed in the immune system; it plays a role in immune cell motility and innate immunity. Mutations in MyoIf may be associated with the loss of hearing. The MyoIf gene has also been found to be fused to the MLL (Mixed lineage leukemia) gene in infant acute myeloid leukemias (AML). SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212761 [Multi-domain]  Cd Length: 53  Bit Score: 114.05  E-value: 1.71e-30
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11827      1 QCKALYAYDAQDTDELSFNEGDIIEILKEDPSGWWTGRLRGKEGLFPGNYVEK 53
SH3 smart00326
Src homology 3 domains; Src homology 3 (SH3) domains bind to target proteins through sequences ...
1079-1132 3.78e-19

Src homology 3 domains; Src homology 3 (SH3) domains bind to target proteins through sequences containing proline and hydrophobic amino acids. Pro-containing polypeptides may bind to SH3 domains in 2 different binding orientations.


Pssm-ID: 214620 [Multi-domain]  Cd Length: 56  Bit Score: 81.82  E-value: 3.78e-19
                            10        20        30        40        50
                    ....*....|....*....|....*....|....*....|....*....|....*
gi 1622892340  1079 GPRCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLH-GQEGLFPGNYVE 1132
Cdd:smart00326    2 GPQVRALYDYTAQDPDELSFKKGDIITVLEKSDDGWWKGRLGrGKEGLFPSNYVE 56
SH3 cd00174
Src Homology 3 domain superfamily; Src Homology 3 (SH3) domains are protein interaction ...
1081-1130 2.68e-17

Src Homology 3 domain superfamily; Src Homology 3 (SH3) domains are protein interaction domains that bind proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. Thus, they are referred to as proline-recognition domains (PRDs). SH3 domains are less selective and show more diverse specificity compared to other PRDs. They have been shown to bind peptide sequences that lack the PxxP motif; examples include the PxxDY motif of Eps8 and the RKxxYxxY sequence in SKAP55. SH3 domain containing proteins play versatile and diverse roles in the cell, including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies, among others. Many members of this superfamily are adaptor proteins that associate with a number of protein partners, facilitating complex formation and signal transduction.


Pssm-ID: 212690 [Multi-domain]  Cd Length: 51  Bit Score: 76.73  E-value: 2.68e-17
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLH-GQEGLFPGNY 1130
Cdd:cd00174      1 YARALYDYEAQDDDELSFKKGDIITVLEKDDDGWWEGELNgGREGLFPANY 51
SH3_CD2AP-like_2 cd11874
Second Src Homology 3 domain (SH3B) of CD2-associated protein and similar proteins; This ...
1081-1132 4.67e-17

Second Src Homology 3 domain (SH3B) of CD2-associated protein and similar proteins; This subfamily is composed of the second SH3 domain (SH3B) of CD2AP, CIN85 (Cbl-interacting protein of 85 kDa), and similar domains. CD2AP and CIN85 are adaptor proteins that bind to protein partners and assemble complexes that have been implicated in T cell activation, kidney function, and apoptosis of neuronal cells. They also associate with endocytic proteins, actin cytoskeleton components, and other adaptor proteins involved in receptor tyrosine kinase (RTK) signaling. CD2AP and the main isoform of CIN85 contain three SH3 domains, a proline-rich region, and a C-terminal coiled-coil domain. All of these domains enable CD2AP and CIN85 to bind various protein partners and assemble complexes that have been implicated in many different functions. SH3B of both proteins have been shown to bind to Cbl. In the case of CD2AP, its SH3B binds to Cbl at a site distinct from the c-Cbl/SH3A binding site. The CIN85 SH3B also binds ubiquitin. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212807 [Multi-domain]  Cd Length: 53  Bit Score: 75.83  E-value: 4.67e-17
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|..
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11874      1 RCKVLFSYTPQNEDELELKVGDTIEVLGEVEEGWWEGKLNGKVGVFPSNFVK 52
SH3_Intersectin_5 cd11840
Fifth Src homology 3 domain (or SH3E) of Intersectin; Intersectins (ITSNs) are adaptor ...
1083-1132 2.45e-15

Fifth Src homology 3 domain (or SH3E) of Intersectin; Intersectins (ITSNs) are adaptor proteins that function in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. They are essential for initiating clathrin-coated pit formation. They bind to many proteins through their multidomain structure and facilitate the assembly of multimeric complexes. Vertebrates contain two ITSN proteins, ITSN1 and ITSN2, which exist in alternatively spliced short and long isoforms. The short isoforms contain two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoforms, in addition, contain RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. ITSN1 and ITSN2 are both widely expressed, with variations depending on tissue type and stage of development. The fifth SH3 domain (or SH3E) of ITSN1 has been shown to bind many protein partners including SGIP1, Sos1, dynamin1/2, CIN85, c-Cbl, SHIP2, N-WASP, and synaptojanin-1, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212774 [Multi-domain]  Cd Length: 53  Bit Score: 70.91  E-value: 2.45e-15
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11840      3 IALFPYTAQNEDELSFQKGDIINVLSKDDPDWWRGELNGQTGLFPSNYVE 52
SH3_CD2AP_2 cd12054
Second Src Homology 3 domain (SH3B) of CD2-associated protein; CD2AP, also called CMS (Cas ...
1081-1134 3.32e-15

Second Src Homology 3 domain (SH3B) of CD2-associated protein; CD2AP, also called CMS (Cas ligand with Multiple SH3 domains) or METS1 (Mesenchyme-to-Epithelium Transition protein with SH3 domains), is a cytosolic adaptor protein that plays a role in regulating the cytoskeleton. It is critical in cell-to-cell union necessary for kidney function. It also stabilizes the contact between a T cell and antigen-presenting cells. It is primarily expressed in podocytes at the cytoplasmic face of the slit diaphragm and serves as a linker anchoring podocin and nephrin to the actin cytoskeleton. CD2AP contains three SH3 domains, a proline-rich region, and a C-terminal coiled-coil domain. All of these domains enable CD2AP to bind various protein partners and assemble complexes that have been implicated in many different functions. This alignment model represents the second SH3 domain (SH3B) of CD2AP. SH3B binds to c-Cbl in a site (TPSSRPLR is the core binding motif) distinct from the c-Cbl/SH3A binding site. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212987 [Multi-domain]  Cd Length: 55  Bit Score: 70.77  E-value: 3.32e-15
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEKI 1134
Cdd:cd12054      2 QCKVLFEYVPQNEDELELKVGDIIDINEEVEEGWWSGTLNGKSGLFPSNFVKEL 55
SH3_Nostrin cd11823
Src homology 3 domain of Nitric Oxide Synthase TRaffic INducer; Nostrin is expressed in ...
1081-1132 4.73e-15

Src homology 3 domain of Nitric Oxide Synthase TRaffic INducer; Nostrin is expressed in endothelial and epithelial cells and is involved in the regulation, trafficking and targeting of endothelial NOS (eNOS). It facilitates the endocytosis of eNOS by coordinating the functions of dynamin and the Wiskott-Aldrich syndrome protein (WASP). Increased expression of Nostrin may be correlated to preeclampsia. Nostrin contains an N-terminal F-BAR domain and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212757 [Multi-domain]  Cd Length: 53  Bit Score: 70.45  E-value: 4.73e-15
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|..
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11823      1 RCKALYSYTANREDELSLQPGDIIEVHEKQDDGWWLGELNGKKGIFPATYVE 52
SH3_OSTF1 cd11772
Src Homology 3 domain of metazoan osteoclast stimulating factor 1; OSTF1, also named OSF or ...
1083-1132 8.09e-15

Src Homology 3 domain of metazoan osteoclast stimulating factor 1; OSTF1, also named OSF or SH3P2, is a signaling protein containing SH3 and ankyrin-repeat domains. It acts through a Src-related pathway to enhance the formation of osteoclasts and bone resorption. It also acts as a negative regulator of cell motility. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212706 [Multi-domain]  Cd Length: 53  Bit Score: 69.64  E-value: 8.09e-15
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11772      3 RALYDYEAQHPDELSFEEGDLLYISDKSDPNWWKATCGGKTGLIPSNYVE 52
SH3_PACSIN cd11843
Src homology 3 domain of Protein kinase C and Casein kinase Substrate in Neurons (PACSIN) ...
1081-1132 1.11e-14

Src homology 3 domain of Protein kinase C and Casein kinase Substrate in Neurons (PACSIN) proteins; PACSINs, also called Synaptic dynamin-associated proteins (Syndapins), act as regulators of cytoskeletal and membrane dynamics. They bind both dynamin and Wiskott-Aldrich syndrome protein (WASP), and may provide direct links between the actin cytoskeletal machinery through WASP and dynamin-dependent endocytosis. Vetebrates harbor three isoforms with distinct expression patterns and specific functions. PACSINs contain an N-terminal F-BAR domain and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212777 [Multi-domain]  Cd Length: 53  Bit Score: 69.37  E-value: 1.11e-14
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILM-EDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11843      1 PVRALYDYEGQESDELSFKAGDILTKLEeEDEQGWCKGRLDGRVGLYPANYVE 53
SH3_PACSIN1-2 cd11998
Src homology 3 domain of Protein kinase C and Casein kinase Substrate in Neurons 1 (PACSIN1) ...
1081-1132 3.69e-14

Src homology 3 domain of Protein kinase C and Casein kinase Substrate in Neurons 1 (PACSIN1) and PACSIN 2; PACSIN 1 or Syndapin I (Synaptic dynamin-associated protein I) is expressed specifically in the brain and is localized in neurites and synaptic boutons. It binds the brain-specific proteins dynamin I, synaptojanin, synapsin I, and neural Wiskott-Aldrich syndrome protein (nWASP), and functions as a link between the cytoskeletal machinery and synaptic vesicle endocytosis. PACSIN 1 interacts with huntingtin and may be implicated in the neuropathology of Huntington's disease. PACSIN 2 or Syndapin II is expressed ubiquitously and is involved in the regulation of tubulin polymerization. It associates with Golgi membranes and forms a complex with dynamin II which is crucial in promoting vesicle formation from the trans-Golgi network. PACSINs act as regulators of cytoskeletal and membrane dynamics. Vetebrates harbor three isoforms with distinct expression patterns and specific functions. PACSINs contain an N-terminal F-BAR domain and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212931 [Multi-domain]  Cd Length: 56  Bit Score: 68.05  E-value: 3.69e-14
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....
gi 1622892340 1081 RCRALYQYVGQDVDELSFNV-NEVIEILMEDSSGWWKGRL-HGQEGLFPGNYVE 1132
Cdd:cd11998      2 RVRALYDYDGQEQDELSFKAgDELTKLEDEDEQGWCKGRLdSGQVGLYPANYVE 55
SH3_Cortactin cd11959
Src homology 3 domain of Cortactin; Cortactin was originally identified as a substrate of Src ...
1084-1132 1.18e-13

Src homology 3 domain of Cortactin; Cortactin was originally identified as a substrate of Src kinase. It is an actin regulatory protein that binds to the Arp2/3 complex and stabilizes branched actin filaments. It is involved in cellular processes that affect cell motility, adhesion, migration, endocytosis, and invasion. It is expressed ubiquitously except in hematopoietic cells, where the homolog hematopoietic lineage cell-specific 1 (HS1) is expressed instead. Cortactin contains an N-terminal acidic domain, several copies of a repeat domain found in cortactin and HS1, a proline-rich region, and a C-terminal SH3 domain. The N-terminal region interacts with the Arp2/3 complex and F-actin, and is crucial in regulating branched actin assembly. Cortactin also serves as a scaffold and provides a bridge to the actin cytoskeleton for membrane trafficking and signaling proteins that bind to its SH3 domain. Binding partners for the SH3 domain of cortactin include dynamin2, N-WASp, MIM, FGD1, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212892 [Multi-domain]  Cd Length: 53  Bit Score: 66.29  E-value: 1.18e-13
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*....
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11959      4 ALYDYQAADDDEISFDPDDIITNIEMIDEGWWRGVCRGKYGLFPANYVE 52
SH3_Abi cd11826
Src homology 3 domain of Abl Interactor proteins; Abl interactor (Abi) proteins are adaptor ...
1083-1132 1.34e-13

Src homology 3 domain of Abl Interactor proteins; Abl interactor (Abi) proteins are adaptor proteins serving as binding partners and substrates of Abl tyrosine kinases. They are involved in regulating actin cytoskeletal reorganization and play important roles in membrane-ruffling, endocytosis, cell motility, and cell migration. They localize to sites of actin polymerization in epithelial adherens junction and immune synapses, as well as to the leading edge of lamellipodia. Vertebrates contain two Abi proteins, Abi1 and Abi2. Abi1 displays a wide expression pattern while Abi2 is highly expressed in the eye and brain. Abi proteins contain a homeobox homology domain, a proline-rich region, and a SH3 domain. The SH3 domain of Abi binds to a PxxP motif in Abl. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212760 [Multi-domain]  Cd Length: 52  Bit Score: 66.19  E-value: 1.34e-13
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11826      3 VALYDYTADKDDELSFQEGDIIYVTKKNDDGWYEGVLNGVTGLFPGNYVE 52
SH3_CIN85_2 cd12055
Second Src Homology 3 domain (SH3B) of Cbl-interacting protein of 85 kDa; CIN85, also called ...
1081-1133 1.39e-13

Second Src Homology 3 domain (SH3B) of Cbl-interacting protein of 85 kDa; CIN85, also called SH3 domain-containing kinase-binding protein 1 (SH3KBP1) or CD2-binding protein 3 (CD2BP3) or Ruk, is an adaptor protein that is involved in the downregulation of receptor tyrosine kinases by facilitating endocytosis through interaction with endophilin-associated ubiquitin ligase Cbl proteins. It is also important in many other cellular processes including vesicle-mediated transport, cytoskeletal remodelling, apoptosis, cell adhesion and migration, and viral infection, among others. CIN85 exists as multiple variants from alternative splicing; the main variant contains three SH3 domains, a proline-rich region, and a C-terminal coiled-coil domain. All of these domains enable CIN85 to bind various protein partners and assemble complexes that have been implicated in many different functions. This alignment model represents the second SH3 domain (SH3B) of CIN85. SH3B has been shown to bind Cbl proline-rich peptides and ubiquitin. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212988 [Multi-domain]  Cd Length: 53  Bit Score: 66.17  E-value: 1.39e-13
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd12055      1 RCQVAFSYLPQNEDELELKVGDIIEVVGEVEEGWWEGVLNGKTGMFPSNFIKE 53
SH3_PACSIN3 cd11997
Src homology 3 domain of Protein kinase C and Casein kinase Substrate in Neurons 3 (PACSIN3); ...
1079-1132 1.45e-13

Src homology 3 domain of Protein kinase C and Casein kinase Substrate in Neurons 3 (PACSIN3); PACSIN 3 or Syndapin III (Synaptic dynamin-associated protein III) is expressed ubiquitously and regulates glucose uptake in adipocytes through its role in GLUT1 trafficking. It also modulates the subcellular localization and stimulus-specific function of the cation channel TRPV4. PACSINs act as regulators of cytoskeletal and membrane dynamics. Vetebrates harbor three isoforms with distinct expression patterns and specific functions. PACSINs contain an N-terminal F-BAR domain and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212930 [Multi-domain]  Cd Length: 56  Bit Score: 66.14  E-value: 1.45e-13
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*.
gi 1622892340 1079 GPRCRALYQYVGQDVDELSFNV-NEVIEILMEDSSGWWKGRL-HGQEGLFPGNYVE 1132
Cdd:cd11997      1 GVRVRALYDYTGQEADELSFKAgEELLKIGEEDEQGWCKGRLlSGRIGLYPANYVE 56
SH3_9 pfam14604
Variant SH3 domain;
1084-1132 1.83e-13

Variant SH3 domain;


Pssm-ID: 434066 [Multi-domain]  Cd Length: 49  Bit Score: 65.72  E-value: 1.83e-13
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*....
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:pfam14604    1 ALYPYEPKDDDELSLQRGDVITVIEESEDGWWEGINTGRTGLVPANYVE 49
SH3_GRAP2_C cd11950
C-terminal Src homology 3 domain of GRB2-related adaptor protein 2; GRAP2 is also called GADS ...
1083-1132 3.16e-13

C-terminal Src homology 3 domain of GRB2-related adaptor protein 2; GRAP2 is also called GADS (GRB2-related adapter downstream of Shc), GrpL, GRB2L, Mona, or GRID (Grb2-related protein with insert domain). It is expressed specifically in the hematopoietic system. It plays an important role in T cell receptor (TCR) signaling by promoting the formation of the SLP-76:LAT complex, which couples the TCR to the Ras pathway. It also has roles in antigen-receptor and tyrosine kinase mediated signaling. GRAP2 is unique from other GRB2-like adaptor proteins in that it can be regulated by caspase cleavage. It contains an N-terminal SH3 domain, a central SH2 domain, and a C-terminal SH3 domain. The C-terminal SH3 domain of GRAP2 binds to different motifs found in substrate peptides including the typical PxxP motif in hematopoietic progenitor kinase 1 (HPK1), the RxxK motif in SLP-76 and HPK1, and the RxxxxK motif in phosphatase-like protein HD-PTP. SH3 domains are protein interaction domains that typically bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212883 [Multi-domain]  Cd Length: 53  Bit Score: 65.23  E-value: 3.16e-13
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11950      3 RALYDFEALEDDELGFNSGDVIEVLDSSNPSWWKGRLHGKLGLFPANYVA 52
SH3_PIX cd11877
Src Homology 3 domain of Pak Interactive eXchange factors; PIX proteins are Rho guanine ...
1083-1132 5.33e-13

Src Homology 3 domain of Pak Interactive eXchange factors; PIX proteins are Rho guanine nucleotide exchange factors (GEFs), which activate small GTPases by exchanging bound GDP for free GTP. They act as GEFs for both Cdc42 and Rac 1, and have been implicated in cell motility, adhesion, neurite outgrowth, and cell polarity. Vertebrates contain two proteins from the PIX subfamily, alpha-PIX and beta-PIX. Alpha-PIX, also called ARHGEF6, is localized in dendritic spines where it regulates spine morphogenesis. Mutations in the ARHGEF6 gene cause X-linked intellectual disability in humans. Beta-PIX play roles in regulating neuroendocrine exocytosis, focal adhesion maturation, cell migration, synaptic vesicle localization, and insulin secretion. PIX proteins contain an N-terminal SH3 domain followed by RhoGEF (also called Dbl-homologous or DH) and Pleckstrin Homology (PH) domains, and a C-terminal leucine-zipper domain for dimerization. The SH3 domain of PIX binds to an atypical PxxxPR motif in p21-activated kinases (PAKs) with high affinity. The binding of PAKs to PIX facilitate the localization of PAKs to focal complexes and also localizes PAKs to PIX targets Cdc43 and Rac, leading to the activation of PAKs. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212810 [Multi-domain]  Cd Length: 53  Bit Score: 64.26  E-value: 5.33e-13
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11877      3 RAKFNFEGTNEDELSFDKGDIITVTQVVEGGWWEGTLNGKTGWFPSNYVK 52
SH3_CD2AP-like_3 cd11875
Third Src Homology 3 domain (SH3C) of CD2-associated protein and similar proteins; This ...
1081-1132 6.58e-13

Third Src Homology 3 domain (SH3C) of CD2-associated protein and similar proteins; This subfamily is composed of the third SH3 domain (SH3C) of CD2AP, CIN85 (Cbl-interacting protein of 85 kDa), and similar domains. CD2AP and CIN85 are adaptor proteins that bind to protein partners and assemble complexes that have been implicated in T cell activation, kidney function, and apoptosis of neuronal cells. They also associate with endocytic proteins, actin cytoskeleton components, and other adaptor proteins involved in receptor tyrosine kinase (RTK) signaling. CD2AP and the main isoform of CIN85 contain three SH3 domains, a proline-rich region, and a C-terminal coiled-coil domain. All of these domains enable CD2AP and CIN85 to bind various protein partners and assemble complexes that have been implicated in many different functions. SH3C of both proteins have been shown to bind to ubiquitin. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212808 [Multi-domain]  Cd Length: 55  Bit Score: 64.29  E-value: 6.58e-13
                           10        20        30        40        50
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDS--SGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11875      1 KARVLFDYEAENEDELTLREGDIVTILSKDCedKGWWKGELNGKRGVFPDNFVE 54
SH3_HS1 cd12073
Src homology 3 domain of Hematopoietic lineage cell-specific protein 1; HS1, also called HCLS1 ...
1084-1132 8.29e-13

Src homology 3 domain of Hematopoietic lineage cell-specific protein 1; HS1, also called HCLS1 (hematopoietic cell-specific Lyn substrate 1), is a cortactin homolog expressed specifically in hematopoietic cells. It is an actin regulatory protein that binds the Arp2/3 complex and stabilizes branched actin filaments. It is required for cell spreading and signaling in lymphocytes. It regulates cytoskeletal remodeling that controls lymphocyte trafficking, and it also affects tissue invasion and infiltration of leukemic B cells. Like cortactin, HS1 contains an N-terminal acidic domain, several copies of a repeat domain found in cortactin and HS1, a proline-rich region, and a C-terminal SH3 domain. The N-terminal region binds the Arp2/3 complex and F-actin, while the C-terminal region acts as an adaptor or scaffold that can connect varied proteins that bind the SH3 domain within the actin network. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 213006 [Multi-domain]  Cd Length: 55  Bit Score: 64.08  E-value: 8.29e-13
                           10        20        30        40        50
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVI-EILMEDSsGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd12073      5 ALYDYQGEGDDEISFDPQETItDIEMVDE-GWWKGTCHGHRGLFPANYVE 53
SH3_SNX9_like cd11763
Src Homology 3 domain of Sorting Nexin 9 and similar proteins; Sorting nexins (SNXs) are Phox ...
1081-1132 1.03e-12

Src Homology 3 domain of Sorting Nexin 9 and similar proteins; Sorting nexins (SNXs) are Phox homology (PX) domain containing proteins that are involved in regulating membrane traffic and protein sorting in the endosomal system. SNXs differ from each other in their lipid-binding specificity, subcellular localization and specific function in the endocytic pathway. This subfamily consists of SH3 domain containing SNXs including SNX9, SNX18, SNX33, and similar proteins. SNX9 is localized to plasma membrane endocytic sites and acts primarily in clathrin-mediated endocytosis, while SNX18 is localized to peripheral endosomal structures, and acts in a trafficking pathway that is clathrin-independent but relies on AP-1 and PACS1. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212697 [Multi-domain]  Cd Length: 55  Bit Score: 63.50  E-value: 1.03e-12
                           10        20        30        40        50
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDS-SGWWKGR-LHGQEGLFPGNYVE 1132
Cdd:cd11763      1 KVRALYDFDSQPSGELSLRAGEVLTITRQDVgDGWLEGRnSRGEVGLFPSSYVE 54
SH3_PSTPIP1 cd11824
Src homology 3 domain of Proline-Serine-Threonine Phosphatase-Interacting Protein 1; PSTPIP1, ...
1083-1133 1.17e-12

Src homology 3 domain of Proline-Serine-Threonine Phosphatase-Interacting Protein 1; PSTPIP1, also called CD2 Binding Protein 1 (CD2BP1), is mainly expressed in hematopoietic cells. It is a binding partner of the cell surface receptor CD2 and PTP-PEST, a tyrosine phosphatase which functions in cell motility and Rac1 regulation. It also plays a role in the activation of the Wiskott-Aldrich syndrome protein (WASP), which couples actin rearrangement and T cell activation. Mutations in the gene encoding PSTPIP1 cause the autoinflammatory disorder known as PAPA (pyogenic sterile arthritis, pyoderma gangrenosum, and acne) syndrome. PSTPIP1 contains an N-terminal F-BAR domain, PEST motifs, and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212758 [Multi-domain]  Cd Length: 53  Bit Score: 63.55  E-value: 1.17e-12
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11824      3 SVLYDYTAQEDDELSISKGDVVAVIEKGEDGWWTVERNGQKGLVPGTYLEK 53
SH3_Cortactin_like cd11819
Src homology 3 domain of Cortactin and related proteins; This subfamily includes cortactin, ...
1081-1132 1.24e-12

Src homology 3 domain of Cortactin and related proteins; This subfamily includes cortactin, Abp1 (actin-binding protein 1), hematopoietic lineage cell-specific protein 1 (HS1), and similar proteins. These proteins are involved in regulating actin dynamics through direct or indirect interaction with the Arp2/3 complex, which is required to initiate actin polymerization. They all contain at least one C-terminal SH3 domain. Cortactin and HS1 bind Arp2/3 and actin through an N-terminal region that contains an acidic domain and several copies of a repeat domain found in cortactin and HS1. Abp1 binds actin via an N-terminal actin-depolymerizing factor (ADF) homology domain. Yeast Abp1 binds Arp2/3 directly through two acidic domains. Mammalian Abp1 does not directly interact with Arp2/3; instead, it regulates actin dynamics indirectly by interacting with dynamin and WASP family proteins. The C-terminal region of these proteins acts as an adaptor or scaffold that can connect membrane trafficking and signaling proteins that bind the SH3 domain within the actin network. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212753 [Multi-domain]  Cd Length: 54  Bit Score: 63.49  E-value: 1.24e-12
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRL-HGQEGLFPGNYVE 1132
Cdd:cd11819      1 RAKALYDYQAAEDNEISFVEGDIITQIEQIDEGWWLGVNaKGQKGLFPANYVE 53
SH3_GRB2_like_C cd11805
C-terminal Src homology 3 domain of Growth factor receptor-bound protein 2 (GRB2) and related ...
1081-1133 1.36e-12

C-terminal Src homology 3 domain of Growth factor receptor-bound protein 2 (GRB2) and related proteins; This family includes the adaptor protein GRB2 and related proteins including Drosophila melanogaster Downstream of receptor kinase (DRK), Caenorhabditis elegans Sex muscle abnormal protein 5 (Sem-5), GRB2-related adaptor protein (GRAP), GRAP2, and similar proteins. Family members contain an N-terminal SH3 domain, a central SH2 domain, and a C-terminal SH3 domain. GRB2/Sem-5/DRK is a critical signaling molecule that regulates the Ras pathway by linking tyrosine kinases to the Ras guanine nucleotide releasing protein Sos (son of sevenless), which converts Ras to the active GTP-bound state. GRAP2 plays an important role in T cell receptor (TCR) signaling by promoting the formation of the SLP-76:LAT complex, which couples the TCR to the Ras pathway. GRAP acts as a negative regulator of T cell receptor (TCR)-induced lymphocyte proliferation by downregulating the signaling to the Ras/ERK pathway. The C-terminal SH3 domains (SH3c) of GRB2 and GRAP2 have been shown to bind to classical PxxP motif ligands, as well as to non-classical motifs. GRB2 SH3c binds Gab2 (Grb2-associated binder 2) through epitopes containing RxxK motifs, while the SH3c of GRAP2 binds to the phosphatase-like protein HD-PTP via a RxxxxK motif. SH3 domains are protein interaction domains that typically bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212739 [Multi-domain]  Cd Length: 53  Bit Score: 63.42  E-value: 1.36e-12
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11805      1 RVQALYDFNPQEPGELEFRRGDIITVLDSSDPDWWKGELRGRVGIFPANYVQP 53
SH3_GRAF-like cd11882
Src Homology 3 domain of GTPase Regulator Associated with Focal adhesion kinase and similar ...
1081-1132 1.84e-12

Src Homology 3 domain of GTPase Regulator Associated with Focal adhesion kinase and similar proteins; This subfamily is composed of Rho GTPase activating proteins (GAPs) with similarity to GRAF. Members contain an N-terminal BAR domain, followed by a Pleckstrin homology (PH) domain, a Rho GAP domain, and a C-terminal SH3 domain. Although vertebrates harbor four Rho GAPs in the GRAF subfamily including GRAF, GRAF2, GRAF3, and Oligophrenin-1 (OPHN1), only three are included in this model. OPHN1 contains the BAR, PH and GAP domains, but not the C-terminal SH3 domain. GRAF and GRAF2 show GAP activity towards RhoA and Cdc42. GRAF influences Rho-mediated cytoskeletal rearrangements and binds focal adhesion kinase. GRAF2 regulates caspase-activated p21-activated protein kinase-2. The SH3 domain of GRAF and GRAF2 binds PKNbeta, a target of the small GTPase Rho. SH3 domains bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs; they play a role in the regulation of enzymes by intramolecular interactions, changing the subcellular localization of signal pathway components and mediate multiprotein complex assemblies.


Pssm-ID: 212815 [Multi-domain]  Cd Length: 54  Bit Score: 63.08  E-value: 1.84e-12
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILME-DSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11882      1 RARALYACKAEDESELSFEPGQIITNVQPsDEPGWLEGTLNGRTGLIPENYVE 53
SH3_Nck_2 cd11766
Second Src Homology 3 domain of Nck adaptor proteins; Nck adaptor proteins regulate actin ...
1081-1133 1.94e-12

Second Src Homology 3 domain of Nck adaptor proteins; Nck adaptor proteins regulate actin cytoskeleton dynamics by linking proline-rich effector molecules to protein tyrosine kinases and phosphorylated signaling intermediates. They contain three SH3 domains and a C-terminal SH2 domain. They function downstream of the PDGFbeta receptor and are involved in Rho GTPase signaling and actin dynamics. Vertebrates contain two Nck adaptor proteins: Nck1 (also called Nckalpha) and Nck2 (also called Nckbeta or Growth factor receptor-bound protein 4, Grb4), which show partly overlapping functions but also bind distinct targets. Their SH3 domains are involved in recruiting downstream effector molecules, such as the N-WASP/Arp2/3 complex, which when activated induces actin polymerization that results in the production of pedestals, or protrusions of the plasma membrane. The second SH3 domain of Nck appears to prefer ligands containing the APxxPxR motif. SH3 domains are protein interaction domains that usually bind to proline-rich ligands with moderate affinity and selectivity, preferentially a PxxP motif. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212700 [Multi-domain]  Cd Length: 53  Bit Score: 62.67  E-value: 1.94e-12
                           10        20        30        40        50
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11766      1 PAVVKFNYEAQREDELSLRKGDRVLVLEKSSDGWWRGECNGQVGWFPSNYVTE 53
SH3_1 pfam00018
SH3 domain; SH3 (Src homology 3) domains are often indicative of a protein involved in signal ...
1083-1127 2.02e-12

SH3 domain; SH3 (Src homology 3) domains are often indicative of a protein involved in signal transduction related to cytoskeletal organization. First described in the Src cytoplasmic tyrosine kinase. The structure is a partly opened beta barrel.


Pssm-ID: 394975 [Multi-domain]  Cd Length: 47  Bit Score: 62.61  E-value: 2.02e-12
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLH-GQEGLFP 1127
Cdd:pfam00018    1 VALYDYTAQEPDELSFKKGDIIIVLEKSEDGWWKGRNKgGKEGLIP 46
SH3_PACSIN_like cd11999
Src homology 3 domain of an unknown subfamily of proteins with similarity to Protein kinase C ...
1079-1132 2.79e-12

Src homology 3 domain of an unknown subfamily of proteins with similarity to Protein kinase C and Casein kinase Substrate in Neurons (PACSIN) proteins; PACSINs, also called Synaptic dynamin-associated proteins (Syndapins), act as regulators of cytoskeletal and membrane dynamics. They bind both dynamin and Wiskott-Aldrich syndrome protein (WASP), and may provide direct links between the actin cytoskeletal machinery through WASP and dynamin-dependent endocytosis. Vetebrates harbor three isoforms with distinct expression patterns and specific functions. PACSINs contain an N-terminal F-BAR domain and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212932 [Multi-domain]  Cd Length: 56  Bit Score: 62.65  E-value: 2.79e-12
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gi 1622892340 1079 GPRCRALYQYVGQDVDELSFNVNE-VIEILMEDSSGWWKG-RLHGQEGLFPGNYVE 1132
Cdd:cd11999      1 GVRVRAVYDYTGQEPDELSFKAGEeLLKVEDEDEQGWCKGvTDGGAVGLYPANYVE 56
SH3_CD2AP_3 cd12056
Third Src Homology 3 domain (SH3C) of CD2-associated protein; CD2AP, also called CMS (Cas ...
1082-1131 4.31e-12

Third Src Homology 3 domain (SH3C) of CD2-associated protein; CD2AP, also called CMS (Cas ligand with Multiple SH3 domains) or METS1 (Mesenchyme-to-Epithelium Transition protein with SH3 domains), is a cytosolic adaptor protein that plays a role in regulating the cytoskeleton. It is critical in cell-to-cell union necessary for kidney function. It also stabilizes the contact between a T cell and antigen-presenting cells. It is primarily expressed in podocytes at the cytoplasmic face of the slit diaphragm and serves as a linker anchoring podocin and nephrin to the actin cytoskeleton. CD2AP contains three SH3 domains, a proline-rich region, and a C-terminal coiled-coil domain. All of these domains enable CD2AP to bind various protein partners and assemble complexes that have been implicated in many different functions. This alignment model represents the third SH3 domain (SH3C) of CD2AP. SH3C has been shown to bind ubiquitin. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212989 [Multi-domain]  Cd Length: 57  Bit Score: 62.15  E-value: 4.31e-12
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gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMEDS--SGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd12056      4 CKALFHYEGTNEDELDFKEGEIILIISKDTgePGWWKGELNGKEGVFPDNFV 55
SH3_FCHSD_2 cd11762
Second Src Homology 3 domain of FCH and double SH3 domains proteins; This group is composed of ...
1082-1132 7.42e-12

Second Src Homology 3 domain of FCH and double SH3 domains proteins; This group is composed of FCH and double SH3 domains protein 1 (FCHSD1) and FCHSD2. These proteins have a common domain structure consisting of an N-terminal F-BAR (FES-CIP4 Homology and Bin/Amphiphysin/Rvs), two SH3, and C-terminal proline-rich domains. They have only been characterized in silico and their functions remain unknown. This group also includes the insect protein, nervous wreck, which acts as a regulator of synaptic growth signaling. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212696 [Multi-domain]  Cd Length: 57  Bit Score: 61.26  E-value: 7.42e-12
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gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMEDSS----GWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11762      2 VRALYDYEAQSDEELSFPEGAIIRILRKDDNgvddGWWEGEFNGRVGVFPSLVVE 56
SH3_Pex13p_fungal cd11771
Src Homology 3 domain of fungal peroxisomal membrane protein Pex13p; Pex13p, located in the ...
1082-1132 1.71e-11

Src Homology 3 domain of fungal peroxisomal membrane protein Pex13p; Pex13p, located in the peroxisomal membrane, contains two transmembrane regions and a C-terminal SH3 domain. It binds to the peroxisomal targeting type I (PTS1) receptor Pex5p and the docking factor Pex14p through its SH3 domain. It is essential for both PTS1 and PTS2 protein import pathways into the peroxisomal matrix. Pex13p binds Pex14p, which contains a PxxP motif, in a classical fashion to the proline-rich ligand binding site of its SH3 domain. It binds the WxxxF/Y motif of Pex5p in a novel site that does not compete with Pex14p binding. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212705 [Multi-domain]  Cd Length: 60  Bit Score: 60.37  E-value: 1.71e-11
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gi 1622892340 1082 CRALYQYVG-QDVDELSFNVNEVIEIL-----MEDSSGWWKGRLH-GQEGLFPGNYVE 1132
Cdd:cd11771      2 CRALYDFTPeNPEMELSLKKGDIVAVLsktdpLGRDSEWWKGRTRdGRIGWFPSNYVE 59
SH3_Intersectin2_5 cd11996
Fifth Src homology 3 domain (or SH3E) of Intersectin-2; Intersectin-2 (ITSN2) is an adaptor ...
1084-1132 1.75e-11

Fifth Src homology 3 domain (or SH3E) of Intersectin-2; Intersectin-2 (ITSN2) is an adaptor protein that functions in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. It plays a role in clathrin-coated pit (CCP) formation. It binds to many proteins through its multidomain structure and facilitate the assembly of multimeric complexes. ITSN2 also functions as a specific GEF for Cdc42 activation in epithelial morphogenesis, and is required in mitotic spindle orientation. It exists in alternatively spliced short and long isoforms. The short isoform contains two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoform, in addition, contains RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. The fifth SH3 domain (or SH3E) of ITSN2 is expected to bind protein partners, similar to ITSN1 which has been shown to bind many protein partners including SGIP1, Sos1, dynamin1/2, CIN85, c-Cbl, SHIP2, N-WASP, and synaptojanin-1, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212929 [Multi-domain]  Cd Length: 54  Bit Score: 60.38  E-value: 1.75e-11
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11996      5 AMYDYTANNEDELSFSKGQLINVLNKDDPDWWQGEINGVTGLFPSNYVK 53
SH3_Intersectin_2 cd11837
Second Src homology 3 domain (or SH3B) of Intersectin; Intersectins (ITSNs) are adaptor ...
1081-1131 1.77e-11

Second Src homology 3 domain (or SH3B) of Intersectin; Intersectins (ITSNs) are adaptor proteins that function in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. They are essential for initiating clathrin-coated pit formation. They bind to many proteins through their multidomain structure and facilitate the assembly of multimeric complexes. Vertebrates contain two ITSN proteins, ITSN1 and ITSN2, which exist in alternatively spliced short and long isoforms. The short isoforms contain two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoforms, in addition, contain RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. ITSN1 and ITSN2 are both widely expressed, with variations depending on tissue type and stage of development. The second SH3 domain (or SH3B) of ITSN1 has been shown to bind WNK and CdGAP. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212771 [Multi-domain]  Cd Length: 53  Bit Score: 60.07  E-value: 1.77e-11
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILmEDSSGWWKGRLH-GQEGLFPGNYV 1131
Cdd:cd11837      1 TATALYPWRAKKENHLSFAKGDIITVL-EQQEMWWFGELEgGEEGWFPKSYV 51
SH3_Intersectin1_5 cd11995
Fifth Src homology 3 domain (or SH3E) of Intersectin-1; Intersectin-1 (ITSN1) is an adaptor ...
1084-1132 1.85e-11

Fifth Src homology 3 domain (or SH3E) of Intersectin-1; Intersectin-1 (ITSN1) is an adaptor protein that functions in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. It plays a role in clathrin-coated pit (CCP) formation. It binds to many proteins through its multidomain structure and facilitate the assembly of multimeric complexes. ITSN1 localizes in membranous organelles, CCPs, the Golgi complex, and may be involved in the cell membrane trafficking system. It exists in alternatively spliced short and long isoforms. The short isoform contains two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoform, in addition, contains RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. The fifth SH3 domain (or SH3E) of ITSN1 has been shown to bind many protein partners including SGIP1, Sos1, dynamin1/2, CIN85, c-Cbl, SHIP2, N-WASP, and synaptojanin-1, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212928 [Multi-domain]  Cd Length: 54  Bit Score: 59.97  E-value: 1.85e-11
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11995      5 GMYDYTAQNDDELAFSKGQIINVLNKEDPDWWKGELNGQVGLFPSNYVK 53
SH3_2 pfam07653
Variant SH3 domain; SH3 (Src homology 3) domains are often indicative of a protein involved in ...
1081-1134 4.12e-11

Variant SH3 domain; SH3 (Src homology 3) domains are often indicative of a protein involved in signal transduction related to cytoskeletal organization. First described in the Src cytoplasmic tyrosine kinase. The structure is a partly opened beta barrel.


Pssm-ID: 429575 [Multi-domain]  Cd Length: 54  Bit Score: 59.15  E-value: 4.12e-11
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEKI 1134
Cdd:pfam07653    1 YGRVIFDYVGTDKNGLTLKKGDVVKVLGKDNDGWWEGETGGRVGLVPSTAVEEI 54
SH3_p47phox_like cd11856
Src homology 3 domains of the p47phox subunit of NADPH oxidase and similar domains; This ...
1083-1133 5.94e-11

Src homology 3 domains of the p47phox subunit of NADPH oxidase and similar domains; This family is composed of the tandem SH3 domains of p47phox subunit of NADPH oxidase and Nox Organizing protein 1 (NoxO1), the four SH3 domains of Tks4 (Tyr kinase substrate with four SH3 domains), the five SH3 domains of Tks5, the SH3 domain of obscurin, Myosin-I, and similar domains. Most members of this group also contain Phox homology (PX) domains, except for obscurin and Myosin-I. p47phox and NoxO1 are regulators of the phagocytic NADPH oxidase complex (also called Nox2 or gp91phox) and nonphagocytic NADPH oxidase Nox1, respectively. They play roles in the activation of their respective NADPH oxidase, which catalyzes the transfer of electrons from NADPH to molecular oxygen to form superoxide. Tks proteins are Src substrates and scaffolding proteins that play important roles in the formation of podosomes and invadopodia, the dynamic actin-rich structures that are related to cell migration and cancer cell invasion. Obscurin is a giant muscle protein that plays important roles in the organization and assembly of the myofibril and the sarcoplasmic reticulum. Type I myosins (Myosin-I) are actin-dependent motors in endocytic actin structures and actin patches. They play roles in membrane traffic in endocytic and secretory pathways, cell motility, and mechanosensing. Myosin-I contains an N-terminal actin-activated ATPase, a phospholipid-binding TH1 (tail homology 1) domain, and a C-terminal extension which includes an F-actin-binding TH2 domain, an SH3 domain, and an acidic peptide that participates in activating the Arp2/3complex. The SH3 domain of myosin-I is required for myosin-I-induced actin polymerization. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212790 [Multi-domain]  Cd Length: 53  Bit Score: 58.80  E-value: 5.94e-11
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11856      3 VAIADYEAQGDDEISLQEGEVVEVLEKNDSGWWYVRKGDKEGWVPASYLEP 53
SH3_FCHSD_1 cd11761
First Src Homology 3 domain of FCH and double SH3 domains proteins; This group is composed of ...
1082-1133 7.34e-11

First Src Homology 3 domain of FCH and double SH3 domains proteins; This group is composed of FCH and double SH3 domains protein 1 (FCHSD1) and FCHSD2. These proteins have a common domain structure consisting of an N-terminal F-BAR (FES-CIP4 Homology and Bin/Amphiphysin/Rvs), two SH3, and C-terminal proline-rich domains. They have only been characterized in silico and their functions remain unknown. This group also includes the insect protein, nervous wreck, which acts as a regulator of synaptic growth signaling. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212695 [Multi-domain]  Cd Length: 57  Bit Score: 58.53  E-value: 7.34e-11
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....
gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILME-DSSGWWKGR-LHGQEGLFPGNYVEK 1133
Cdd:cd11761      4 CKVLYSYEAQRPDELTITEGEELEVIEDgDGDGWVKARnKSGEVGYVPENYLQF 57
SH3_Abp1_eu cd11960
Src homology 3 domain of eumetazoan Actin-binding protein 1; Abp1, also called drebrin-like ...
1081-1132 8.97e-11

Src homology 3 domain of eumetazoan Actin-binding protein 1; Abp1, also called drebrin-like protein, is an adaptor protein that functions in receptor-mediated endocytosis and vesicle trafficking. It contains an N-terminal actin-binding module, the actin-depolymerizing factor (ADF) homology domain, a helical domain, and a C-terminal SH3 domain. Mammalian Abp1, unlike yeast Abp1, does not contain an acidic domain that interacts with the Arp2/3 complex. It regulates actin dynamics indirectly by interacting with dynamin and WASP family proteins. Abp1 deficiency causes abnormal organ structure and function of the spleen, heart, and lung of mice. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212893 [Multi-domain]  Cd Length: 54  Bit Score: 58.18  E-value: 8.97e-11
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRL-HGQEGLFPGNYVE 1132
Cdd:cd11960      1 RARALYDYQAADDTEISFDPGDIITDIEQIDEGWWRGTGpDGTYGLFPANYVE 53
SH3_PLCgamma cd11825
Src homology 3 domain of Phospholipase C (PLC) gamma; PLC catalyzes the hydrolysis of ...
1082-1133 1.05e-10

Src homology 3 domain of Phospholipase C (PLC) gamma; PLC catalyzes the hydrolysis of phosphatidylinositol (4,5)-bisphosphate [PtdIns(4,5)P2] to produce Ins(1,4,5)P3 and diacylglycerol (DAG) in response to various receptors. Ins(1,4,5)P3 initiates the calcium signaling cascade while DAG functions as an activator of PKC. PLCgamma catalyzes this reaction in tyrosine kinase-dependent signaling pathways. It is activated and recruited to its substrate at the membrane. Vertebrates contain two forms of PLCgamma, PLCgamma1, which is widely expressed, and PLCgamma2, which is primarily found in haematopoietic cells. PLCgamma contains a Pleckstrin homology (PH) domain followed by an elongation factor (EF) domain, two catalytic regions of PLC domains that flank two tandem SH2 domains, followed by a SH3 domain and C2 domain. The SH3 domain of PLCgamma1 directly interacts with dynamin-1 and can serve as a guanine nucleotide exchange factor (GEF). It also interacts with Cbl, inhibiting its phosphorylation and activity. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212759 [Multi-domain]  Cd Length: 54  Bit Score: 58.11  E-value: 1.05e-10
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQ-EGLFPGNYVEK 1133
Cdd:cd11825      2 VKALYDYRAQRPDELSFCKHAIITNVEKEDGGWWRGDYGGKkQKWFPANYVEE 54
SH3_D21-like cd12142
Src Homology 3 domain of SH3 domain-containing protein 21 (SH3D21) and similar proteins; ...
1082-1132 1.12e-10

Src Homology 3 domain of SH3 domain-containing protein 21 (SH3D21) and similar proteins; N-terminal SH3 domain of the uncharacterized protein SH3 domain-containing protein 21, and similar uncharacterized domains, it belongs to the CD2AP-like_3 subfamily of proteins. The CD2AP-like_3 subfamily is composed of the third SH3 domain (SH3C) of CD2AP, CIN85 (Cbl-interacting protein of 85 kDa), and similar domains. CD2AP and CIN85 are adaptor proteins that bind to protein partners and assemble complexes that have been implicated in T cell activation, kidney function, and apoptosis of neuronal cells. They also associate with endocytic proteins, actin cytoskeleton components, and other adaptor proteins involved in receptor tyrosine kinase (RTK) signaling. CD2AP and the main isoform of CIN85 contain three SH3 domains, a proline-rich region, and a C-terminal coiled-coil domain. All of these domains enable CD2AP and CIN85 to bind various protein partners and assemble complexes that have been implicated in many different functions. SH3C of both proteins have been shown to bind to ubiquitin. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 213018 [Multi-domain]  Cd Length: 55  Bit Score: 57.86  E-value: 1.12e-10
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMEDSS--GWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd12142      2 CRVLFDYNPVAPDELALKKGDVIEVISKETEdeGWWEGELNGRRGFFPDNFVM 54
SH3_Intersectin_1 cd11836
First Src homology 3 domain (or SH3A) of Intersectin; Intersectins (ITSNs) are adaptor ...
1081-1133 1.64e-10

First Src homology 3 domain (or SH3A) of Intersectin; Intersectins (ITSNs) are adaptor proteins that function in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. They are essential for initiating clathrin-coated pit formation. They bind to many proteins through their multidomain structure and facilitate the assembly of multimeric complexes. Vertebrates contain two ITSN proteins, ITSN1 and ITSN2, which exist in alternatively spliced short and long isoforms. The short isoforms contain two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoforms, in addition, contain RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. ITSN1 and ITSN2 are both widely expressed, with variations depending on tissue type and stage of development. The first SH3 domain (or SH3A) of ITSN1 has been shown to bind many proteins including Sos1, dynamin1/2, CIN85, c-Cbl, PI3K-C2, SHIP2, N-WASP, and CdGAP, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212770 [Multi-domain]  Cd Length: 55  Bit Score: 57.37  E-value: 1.64e-10
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSS--GWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11836      1 KYRALYAFEARNPDEISFQPGDIIQVDESQVAepGWLAGELKGKTGWFPANYVEK 55
SH3_Abp1_fungi_C2 cd11961
Second C-terminal Src homology 3 domain of Fungal Actin-binding protein 1; Abp1 is an adaptor ...
1083-1132 1.79e-10

Second C-terminal Src homology 3 domain of Fungal Actin-binding protein 1; Abp1 is an adaptor protein that functions in receptor-mediated endocytosis and vesicle trafficking. It contains an N-terminal actin-binding module, the actin-depolymerizing factor (ADF) homology domain, a central proline-rich region, and a C-terminal SH3 domain (many yeast Abp1 proteins contain two C-terminal SH3 domains). Yeast Abp1 also contains two acidic domains that bind directly to the Arp2/3 complex, which is required to initiate actin polymerization. The SH3 domain of yeast Abp1 binds and localizes the kinases, Ark1p and Prk1p, which facilitate actin patch disassembly following vesicle internalization. It also mediates the localization to the actin patch of the synaptojanin-like protein, Sjl2p, which plays a key role in endocytosis. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212894 [Multi-domain]  Cd Length: 53  Bit Score: 57.15  E-value: 1.79e-10
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1083 RALYQYVGQDVDELSFNVNE-VIEILMEDSSgWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11961      3 KALYDYDAAEDNELSFFENDkIINIEFVDDD-WWLGECHGSRGLFPSNYVE 52
SH3_GRB2_C cd11949
C-terminal Src homology 3 domain of Growth factor receptor-bound protein 2; GRB2 is a critical ...
1083-1132 3.39e-10

C-terminal Src homology 3 domain of Growth factor receptor-bound protein 2; GRB2 is a critical signaling molecule that regulates the Ras pathway by linking tyrosine kinases to the Ras guanine nucleotide releasing protein Sos (son of sevenless), which converts Ras to the active GTP-bound state. It is ubiquitously expressed in all tissues throughout development and is important in cell cycle progression, motility, morphogenesis, and angiogenesis. In lymphocytes, GRB2 is associated with antigen receptor signaling components. GRB2 contains an N-terminal SH3 domain, a central SH2 domain, and a C-terminal SH3 domain. The C-terminal SH3 domain of GRB2 binds to Gab2 (Grb2-associated binder 2) through epitopes containing RxxK motifs, as well as to the proline-rich C-terminus of FGRF2. SH3 domains are protein interaction domains that typically bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212882 [Multi-domain]  Cd Length: 53  Bit Score: 56.39  E-value: 3.39e-10
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11949      3 QALFDFDPQEDGELGFRRGDFIEVMDNSDPNWWKGACHGQTGMFPRNYVT 52
SH3_STAM cd11820
Src homology 3 domain of Signal Transducing Adaptor Molecules; STAMs were discovered as ...
1081-1133 5.03e-10

Src homology 3 domain of Signal Transducing Adaptor Molecules; STAMs were discovered as proteins that are highly phosphorylated following cytokine and growth factor stimulation. They function in cytokine signaling and surface receptor degradation, as well as regulate Golgi morphology. They associate with many proteins including Jak2 and Jak3 tyrosine kinases, Hrs, AMSH, and UBPY. STAM adaptor proteins contain VHS (Vps27, Hrs, STAM homology), ubiquitin interacting (UIM), and SH3 domains. There are two vertebrate STAMs, STAM1 and STAM2, which may be functionally redundant; vertebrate STAMs contain ITAM motifs. They are part of the endosomal sorting complex required for transport (ESCRT-0). STAM2 deficiency in mice did not cause any obvious abnormality, while STAM1 deficiency resulted in growth retardation. Loss of both STAM1 and STAM2 in mice proved lethal, indicating that STAMs are important for embryonic development. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212754 [Multi-domain]  Cd Length: 54  Bit Score: 55.93  E-value: 5.03e-10
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11820      2 KVRALYDFEAAEDNELTFKAGEIITVLDDSDPNWWKGSNHRGEGLFPANFVTA 54
SH3_SH3YL1_like cd11841
Src homology 3 domain of SH3 domain containing Ysc84-like 1 (SH3YL1) protein; SH3YL1 localizes ...
1084-1131 5.29e-10

Src homology 3 domain of SH3 domain containing Ysc84-like 1 (SH3YL1) protein; SH3YL1 localizes to the plasma membrane and is required for dorsal ruffle formation. It binds phosphoinositides (PIs) with high affinity through its N-terminal SYLF domain (also called DUF500). In addition, SH3YL1 contains a C-terminal SH3 domain which has been reported to bind to N-WASP, dynamin 2, and SHIP2 (a PI 5-phosphatase). SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212775  Cd Length: 54  Bit Score: 55.86  E-value: 5.29e-10
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSS--GWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11841      4 ALYSFEGQQPCDLSFQAGDRITVLTRTDSqfDWWEGRLRGRVGIFPANYV 53
SH3_Endophilin_A cd11803
Src homology 3 domain of Endophilin-A; Endophilins play roles in synaptic vesicle formation, ...
1080-1132 7.46e-10

Src homology 3 domain of Endophilin-A; Endophilins play roles in synaptic vesicle formation, virus budding, mitochondrial morphology maintenance, receptor-mediated endocytosis inhibition, and endosomal sorting. They are classified into two types, A and B. Vertebrates contain three endophilin-A isoforms (A1, A2, and A3). Endophilin-A proteins are enriched in the brain and play multiple roles in receptor-mediated endocytosis. They tubulate membranes and regulate calcium influx into neurons to trigger the activation of the endocytic machinery. They are also involved in the sorting of plasma membrane proteins, actin filament assembly, and the uncoating of clathrin-coated vesicles for fusion with endosomes. Endophilins contain an N-terminal N-BAR domain (BAR domain with an additional N-terminal amphipathic helix), followed by a variable region containing proline clusters, and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212737 [Multi-domain]  Cd Length: 55  Bit Score: 55.73  E-value: 7.46e-10
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1080 PRCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11803      1 PCCRALYDFEPENEGELGFKEGDIITLTNQIDENWYEGMVNGQSGFFPVNYVE 53
SH3_betaPIX cd12061
Src Homology 3 domain of beta-Pak Interactive eXchange factor; Beta-PIX, also called Rho ...
1083-1134 8.04e-10

Src Homology 3 domain of beta-Pak Interactive eXchange factor; Beta-PIX, also called Rho guanine nucleotide exchange factor 7 (ARHGEF7) or Cool (Cloned out of Library)-1, activates small GTPases by exchanging bound GDP for free GTP. It acts as a GEF for both Cdc42 and Rac 1, and plays important roles in regulating neuroendocrine exocytosis, focal adhesion maturation, cell migration, synaptic vesicle localization, and insulin secretion. PIX proteins contain an N-terminal SH3 domain followed by RhoGEF (also called Dbl-homologous or DH) and Pleckstrin Homology (PH) domains, and a C-terminal leucine-zipper domain for dimerization. The SH3 domain of PIX binds to an atypical PxxxPR motif in p21-activated kinases (PAKs) with high affinity. The binding of PAKs to PIX facilitate the localization of PAKs to focal complexes and also localizes PAKs to PIX targets Cdc43 and Rac, leading to the activation of PAKs. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212994 [Multi-domain]  Cd Length: 54  Bit Score: 55.46  E-value: 8.04e-10
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|..
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEKI 1134
Cdd:cd12061      3 RAKFNFQQTNEDELSFSKGDVIHVTRVEEGGWWEGTHNGRTGWFPSNYVREI 54
SH3_Abi2 cd11972
Src homology 3 domain of Abl Interactor 2; Abi2 is highly expressed in the brain and eye. It ...
1084-1134 1.06e-09

Src homology 3 domain of Abl Interactor 2; Abi2 is highly expressed in the brain and eye. It regulates actin cytoskeletal reorganization at adherens junctions and dendritic spines, which is important in cell morphogenesis, migration, and cognitive function. Mice deficient with Abi2 show defects in orientation and migration of lens fibers, neuronal migration, dendritic spine morphology, as well as deficits in learning and memory. Abi proteins are adaptor proteins serving as binding partners and substrates of Abl tyrosine kinases. They are involved in regulating actin cytoskeletal reorganization and play important roles in membrane-ruffling, endocytosis, cell motility, and cell migration. Abi proteins contain a homeobox homology domain, a proline-rich region, and a SH3 domain. The SH3 domain of Abi binds to a PxxP motif in Abl. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212905 [Multi-domain]  Cd Length: 61  Bit Score: 55.40  E-value: 1.06e-09
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEKI 1134
Cdd:cd11972      7 AIYDYTKDKEDELSFQEGAIIYVIKKNDDGWYEGVMNGVTGLFPGNYVESI 57
SH3_GRAP_N cd11948
N-terminal Src homology 3 domain of GRB2-related adaptor protein; GRAP is a GRB-2 like adaptor ...
1084-1132 1.94e-09

N-terminal Src homology 3 domain of GRB2-related adaptor protein; GRAP is a GRB-2 like adaptor protein that is highly expressed in lymphoid tissues. It acts as a negative regulator of T cell receptor (TCR)-induced lymphocyte proliferation by downregulating the signaling to the Ras/ERK pathway. It has been identified as a regulator of TGFbeta signaling in diabetic kidney tubules and may have a role in the pathogenesis of the disease. GRAP contains an N-terminal SH3 domain, a central SH2 domain, and a C-terminal SH3 domain. The N-terminal SH3 domain of the related protein GRB2 binds to Sos and Sos-derived proline-rich peptides. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212881 [Multi-domain]  Cd Length: 54  Bit Score: 54.44  E-value: 1.94e-09
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEIL-MEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11948      4 ALYSFQATESDELPFQKGDILKILnMEDDQNWYKAELQGREGYIPKNYIK 53
SH3_Eve1_4 cd11817
Fourth Src homology 3 domain of ADAM-binding protein Eve-1; Eve-1, also called SH3 ...
1082-1130 2.05e-09

Fourth Src homology 3 domain of ADAM-binding protein Eve-1; Eve-1, also called SH3 domain-containing protein 19 (SH3D19) or EEN-binding protein (EBP), exists in multiple alternatively spliced isoforms. The longest isoform contains five SH3 domain in the C-terminal region and seven proline-rich motifs in the N-terminal region. It is abundantly expressed in skeletal muscle and heart, and may be involved in regulating the activity of ADAMs (A disintegrin and metalloproteases). Eve-1 interacts with EEN, an endophilin involved in endocytosis and may be the target of the MLL-EEN fusion protein that is implicated in leukemogenesis. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212751 [Multi-domain]  Cd Length: 50  Bit Score: 54.02  E-value: 2.05e-09
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*....
gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNY 1130
Cdd:cd11817      2 AVALYDFTGETEEDLSFQRGDRILVTEHLDAEWSRGRLNGREGIFPRAF 50
SH3_Bzz1_2 cd11778
Second Src Homology 3 domain of Bzz1 and similar domains; Bzz1 (or Bzz1p) is a WASP ...
1084-1130 2.10e-09

Second Src Homology 3 domain of Bzz1 and similar domains; Bzz1 (or Bzz1p) is a WASP/Las17-interacting protein involved in endocytosis and trafficking to the vacuole. It physically interacts with type I myosins and functions in the early steps of endocytosis. Together with other proteins, it induces membrane scission in yeast. Bzz1 contains an N-terminal F-BAR (FES-CIP4 Homology and Bin/Amphiphysin/Rvs), a central coiled-coil, and two C-terminal SH3 domains. This model represents the second C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212712 [Multi-domain]  Cd Length: 51  Bit Score: 54.04  E-value: 2.10e-09
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*...
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDS-SGWWKGRLHGQEGLFPGNY 1130
Cdd:cd11778      4 ALYDYEAQGDDEISIRVGDRIAVIRGDDgSGWTYGEINGVKGLFPTSY 51
SH3_AHI-1 cd11812
Src Homology 3 domain of Abelson helper integration site-1 (AHI-1); AHI-1, also called ...
1084-1131 2.17e-09

Src Homology 3 domain of Abelson helper integration site-1 (AHI-1); AHI-1, also called Jouberin, is expressed in high levels in the brain, gonad tissues, and skeletal muscle. It is an adaptor protein that interacts with the small GTPase Rab8a and regulates it distribution and function, affecting cilium formation and vesicle transport. Mutations in the AHI-1 gene can cause Joubert syndrome, a disorder characterized by brainstem malformations, cerebellar aplasia/hypoplasia, and retinal dystrophy. AHI-1 variation is also associated with susceptibility to schizophrenia and type 2 diabetes mellitus progression. AHI-1 contains WD40 and SH3 domains. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212746 [Multi-domain]  Cd Length: 52  Bit Score: 54.05  E-value: 2.17e-09
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRL-HGQEGLFPGNYV 1131
Cdd:cd11812      4 ALYDYTANRSDELTIHRGDIIRVLYKDNDNWWFGSLvNGQQGYFPANYV 52
SH3_VAV1_2 cd11976
C-terminal (or second) Src homology 3 domain of VAV1 protein; VAV1 is expressed predominantly ...
1083-1133 2.34e-09

C-terminal (or second) Src homology 3 domain of VAV1 protein; VAV1 is expressed predominantly in the hematopoietic system and it plays an important role in the development and activation of B and T cells. It is activated by tyrosine phosphorylation to function as a guanine nucleotide exchange factor (GEF) for Rho GTPases following cell surface receptor activation, triggering various effects such as cytoskeletal reorganization, transcription regulation, cell cycle progression, and calcium mobilization. It also serves as a scaffold protein and has been shown to interact with Ku70, Socs1, Janus kinase 2, SIAH2, S100B, Abl gene, ZAP-70, SLP76, and Syk, among others. VAV proteins contain several domains that enable their function: N-terminal calponin homology (CH), acidic, RhoGEF (also called Dbl-homologous or DH), Pleckstrin Homology (PH), C1 (zinc finger), SH2, and two SH3 domains. The C-terminal SH3 domain of Vav1 interacts with a wide variety of proteins including cytoskeletal regulators (zyxin), RNA-binding proteins (Sam68), transcriptional regulators, viral proteins, and dynamin 2. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212909 [Multi-domain]  Cd Length: 54  Bit Score: 54.18  E-value: 2.34e-09
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDS-SGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11976      3 KARYDFCARDRSELSLKEGDIIKILNKKGqQGWWRGEIYGRVGWFPANYVEE 54
SH3_Sdc25 cd11883
Src Homology 3 domain of Sdc25/Cdc25 guanine nucleotide exchange factors; This subfamily is ...
1082-1130 2.62e-09

Src Homology 3 domain of Sdc25/Cdc25 guanine nucleotide exchange factors; This subfamily is composed of the Saccharomyces cerevisiae guanine nucleotide exchange factors (GEFs) Sdc25 and Cdc25, and similar proteins. These GEFs regulate Ras by stimulating the GDP/GTP exchange on Ras. Cdc25 is involved in the Ras/PKA pathway that plays an important role in the regulation of metabolism, stress responses, and proliferation, depending on available nutrients and conditions. Proteins in this subfamily contain an N-terminal SH3 domain as well as REM (Ras exchanger motif) and RasGEF domains at the C-terminus. SH3 domains bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs; they play a role in the regulation of enzymes by intramolecular interactions, changing the subcellular localization of signal pathway components and mediate multiprotein complex assemblies.


Pssm-ID: 212816  Cd Length: 55  Bit Score: 54.21  E-value: 2.62e-09
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gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKG-----RLHGQEGLFPGNY 1130
Cdd:cd11883      2 VVALYDFTPKSKNQLSFKAGDIIYVLNKDPSGWWDGviissSGKVKRGWFPSNY 55
SH3_MLK4 cd12058
Src Homology 3 domain of Mixed Lineage Kinase 4; MLK4 is a Serine/Threonine Kinase (STK), ...
1084-1131 2.81e-09

Src Homology 3 domain of Mixed Lineage Kinase 4; MLK4 is a Serine/Threonine Kinase (STK), catalyzing the transfer of the gamma-phosphoryl group from ATP to S/T residues on protein substrates. MLKs act as mitogen-activated protein kinase kinase kinases (MAP3Ks, MKKKs, MAPKKKs), which phosphorylate and activate MAPK kinases (MAPKKs or MKKs or MAP2Ks), which in turn phosphorylate and activate MAPKs during signaling cascades that are important in mediating cellular responses to extracellular signals. MLKs play roles in immunity and inflammation, as well as in cell death, proliferation, and cell cycle regulation. The specific function of MLK4 is yet to be determined. Mutations in the kinase domain of MLK4 have been detected in colorectal cancers. MLK4 contains an SH3 domain, a catalytic kinase domain, a leucine zipper, a proline-rich region, and a CRIB domain that mediates binding to GTP-bound Cdc42 and Rac. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212991 [Multi-domain]  Cd Length: 58  Bit Score: 54.18  E-value: 2.81e-09
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSS-----GWWKGRLHGQEGLFPGNYV 1131
Cdd:cd12058      4 ALYDYEASGEDELSLRRGDVVEVLSQDAAvsgddGWWAGKIRHRLGIFPANYV 56
SH3_CIN85_1 cd12052
First Src Homology 3 domain (SH3A) of Cbl-interacting protein of 85 kDa; CIN85, also called ...
1086-1133 3.26e-09

First Src Homology 3 domain (SH3A) of Cbl-interacting protein of 85 kDa; CIN85, also called SH3 domain-containing kinase-binding protein 1 (SH3KBP1) or CD2-binding protein 3 (CD2BP3) or Ruk, is an adaptor protein that is involved in the downregulation of receptor tyrosine kinases by facilitating endocytosis through interaction with endophilin-associated ubiquitin ligase Cbl proteins. It is also important in many other cellular processes including vesicle-mediated transport, cytoskeletal remodelling, apoptosis, cell adhesion and migration, and viral infection, among others. CIN85 exists as multiple variants from alternative splicing; the main variant contains three SH3 domains, a proline-rich region, and a C-terminal coiled-coil domain. All of these domains enable CIN85 to bind various protein partners and assemble complexes that have been implicated in many different functions. This alignment model represents the first SH3 domain (SH3A) of CIN85; SH3A binds to internal proline-rich motifs within the proline-rich region. This intramolecular interaction serves as a regulatory mechanism to keep CIN85 in a closed conformation, preventing the recruitment of other proteins. SH3A has also been shown to bind ubiquitin and to an atypical PXXXPR motif at the C-terminus of Cbl and the cytoplasmic end of the cell adhesion protein CD2. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212985 [Multi-domain]  Cd Length: 53  Bit Score: 53.74  E-value: 3.26e-09
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gi 1622892340 1086 YQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd12052      6 FDYKAQHEDELTITVGDIITKIKKDDGGWWEGEIKGRRGLFPDNFVRE 53
SH3_SH3RF_1 cd11786
First Src Homology 3 domain of SH3 domain containing ring finger proteins; This model ...
1083-1132 3.45e-09

First Src Homology 3 domain of SH3 domain containing ring finger proteins; This model represents the first SH3 domain of SH3RF1 (or POSH), SH3RF2 (or POSHER), SH3RF3 (POSH2), and similar domains. Members of this family are scaffold proteins that function as E3 ubiquitin-protein ligases. They all contain an N-terminal RING finger domain and multiple SH3 domains; SH3RF1 and SH3RF3 have four SH3 domains while SH3RF2 has three. SH3RF1 plays a role in calcium homeostasis through the control of the ubiquitin domain protein Herp. It may also have a role in regulating death receptor mediated and JNK mediated apoptosis. SH3RF3 interacts with p21-activated kinase 2 (PAK2) and GTP-loaded Rac1. It may play a role in regulating JNK mediated apoptosis in certain conditions. SH3RF2 acts as an anti-apoptotic regulator of the JNK pathway by binding to and promoting the degradation of SH3RF1. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212720 [Multi-domain]  Cd Length: 53  Bit Score: 53.52  E-value: 3.45e-09
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11786      3 KALYNYEGKEPGDLSFKKGDIILLRKRIDENWYHGECNGKQGFFPASYVQ 52
SH3_STAM2 cd11963
Src homology 3 domain of Signal Transducing Adaptor Molecule 2; STAM2, also called EAST ...
1081-1131 3.58e-09

Src homology 3 domain of Signal Transducing Adaptor Molecule 2; STAM2, also called EAST (Epidermal growth factor receptor-associated protein with SH3 and TAM domain) or Hbp (Hrs binding protein), is part of the endosomal sorting complex required for transport (ESCRT-0). It plays a role in sorting mono-ubiquinated endosomal cargo for trafficking to the lysosome for degradation. It is also involved in the regulation of exocytosis. STAMs were discovered as proteins that are highly phosphorylated following cytokine and growth factor stimulation. They function in cytokine signaling and surface receptor degradation, as well as regulate Golgi morphology. They associate with many proteins including Jak2 and Jak3 tyrosine kinases, Hrs, AMSH, and UBPY. STAM adaptor proteins contain VHS (Vps27, Hrs, STAM homology), ubiquitin interacting (UIM), and SH3 domains. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212896 [Multi-domain]  Cd Length: 57  Bit Score: 53.87  E-value: 3.58e-09
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11963      3 KVRALYDFEAVEDNELTFKHGEIIIVLDDSDANWWKGENHRGVGLFPSNFV 53
SH3_Ysc84p_like cd11842
Src homology 3 domain of Ysc84p and similar fungal proteins; This family is composed of the ...
1081-1132 3.87e-09

Src homology 3 domain of Ysc84p and similar fungal proteins; This family is composed of the Saccharomyces cerevisiae proteins, Ysc84p (also called LAS17-binding protein 4, Lsb4p) and Lsb3p, and similar fungal proteins. They contain an N-terminal SYLF domain (also called DUF500) and a C-terminal SH3 domain. Ysc84p localizes to actin patches and plays an important in actin polymerization during endocytosis. The N-terminal domain of both Ysc84p and Lsb3p can bind and bundle actin filaments. A study of the yeast SH3 domain interactome predicts that the SH3 domains of Lsb3p and Lsb4p may function as molecular hubs for the assembly of endocytic complexes. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212776 [Multi-domain]  Cd Length: 55  Bit Score: 53.58  E-value: 3.87e-09
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSG--WWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11842      1 KAVALYDFAGEQPGDLAFQKGDIITILKKSDSQndWWTGRIGGREGIFPANYVE 54
SH3_PLCgamma1 cd11970
Src homology 3 domain of Phospholipase C (PLC) gamma 1; PLCgamma1 is widely expressed and is ...
1083-1134 4.07e-09

Src homology 3 domain of Phospholipase C (PLC) gamma 1; PLCgamma1 is widely expressed and is essential in growth and development. It is activated by the TrkA receptor tyrosine kinase and functions as a key regulator of cell differentiation. It is also the predominant PLCgamma in T cells and is required for T cell and NK cell function. PLCs catalyze the hydrolysis of phosphatidylinositol (4,5)-bisphosphate [PtdIns(4,5)P2] to produce Ins(1,4,5)P3 and diacylglycerol (DAG). Ins(1,4,5)P3 initiates the calcium signaling cascade while DAG functions as an activator of PKC. PLCgamma contains a Pleckstrin homology (PH) domain followed by an elongation factor (EF) domain, two catalytic regions of PLC domains that flank two tandem SH2 domains, followed by a SH3 domain and C2 domain. The SH3 domain of PLCgamma1 directly interacts with dynamin-1 and can serve as a guanine nucleotide exchange factor (GEF). It also interacts with Cbl, inhibiting its phosphorylation and activity. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212903  Cd Length: 60  Bit Score: 53.84  E-value: 4.07e-09
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGL-FPGNYVEKI 1134
Cdd:cd11970      7 KALFDYKAQREDELTFTKNAIIQNVEKQEGGWWRGDYGGKKQLwFPSNYVEEI 59
SH3_CIN85_3 cd12057
Third Src Homology 3 domain (SH3C) of Cbl-interacting protein of 85 kDa; CIN85, also called ...
1082-1132 4.18e-09

Third Src Homology 3 domain (SH3C) of Cbl-interacting protein of 85 kDa; CIN85, also called SH3 domain-containing kinase-binding protein 1 (SH3KBP1) or CD2-binding protein 3 (CD2BP3) or Ruk, is an adaptor protein that is involved in the downregulation of receptor tyrosine kinases by facilitating endocytosis through interaction with endophilin-associated ubiquitin ligase Cbl proteins. It is also important in many other cellular processes including vesicle-mediated transport, cytoskeletal remodelling, apoptosis, cell adhesion and migration, and viral infection, among others. CIN85 exists as multiple variants from alternative splicing; the main variant contains three SH3 domains, a proline-rich region, and a C-terminal coiled-coil domain. All of these domains enable CIN85 to bind various protein partners and assemble complexes that have been implicated in many different functions. This alignment model represents the third SH3 domain (SH3C) of CIN85. SH3C has been shown to bind ubiquitin. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212990 [Multi-domain]  Cd Length: 56  Bit Score: 53.36  E-value: 4.18e-09
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gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMED--SSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd12057      2 CKVLFPYEAQNEDELTIKEGDIVTLISKDciDAGWWEGELNGRRGVFPDNFVK 54
SH3_STAM1 cd11964
Src homology 3 domain of Signal Transducing Adaptor Molecule 1; STAM1 is part of the endosomal ...
1081-1131 4.88e-09

Src homology 3 domain of Signal Transducing Adaptor Molecule 1; STAM1 is part of the endosomal sorting complex required for transport (ESCRT-0) and is involved in sorting ubiquitinated cargo proteins from the endosome. It may also be involved in the regulation of IL2 and GM-CSF mediated signaling, and has been implicated in neural cell survival. STAMs were discovered as proteins that are highly phosphorylated following cytokine and growth factor stimulation. They function in cytokine signaling and surface receptor degradation, as well as regulate Golgi morphology. They associate with many proteins including Jak2 and Jak3 tyrosine kinases, Hrs, AMSH, and UBPY. STAM adaptor proteins contain VHS (Vps27, Hrs, STAM homology), ubiquitin interacting (UIM), and SH3 domains. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212897 [Multi-domain]  Cd Length: 55  Bit Score: 53.41  E-value: 4.88e-09
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11964      2 KVRAIYDFEAAEDNELTFKAGDIITILDDSDPNWWKGETPQGTGLFPSNFV 52
SH3_Abi1 cd11971
Src homology 3 domain of Abl Interactor 1; Abi1, also called e3B1, is a central regulator of ...
1084-1134 5.30e-09

Src homology 3 domain of Abl Interactor 1; Abi1, also called e3B1, is a central regulator of actin cytoskeletal reorganization through interactions with many protein complexes. It is part of WAVE, a nucleation-promoting factor complex, that links Rac 1 activation to actin polymerization causing lamellipodia protrusion at the plasma membrane. Abi1 interact with formins to promote protrusions at the leading edge of motile cells. It also is a target of alpha4 integrin, regulating membrane protrusions at sites of integrin engagement. Abi proteins are adaptor proteins serving as binding partners and substrates of Abl tyrosine kinases. They are involved in regulating actin cytoskeletal reorganization and play important roles in membrane-ruffling, endocytosis, cell motility, and cell migration. Abi proteins contain a homeobox homology domain, a proline-rich region, and a SH3 domain. The SH3 domain of Abi binds to a PxxP motif in Abl. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212904 [Multi-domain]  Cd Length: 59  Bit Score: 53.49  E-value: 5.30e-09
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEKI 1134
Cdd:cd11971      4 AIYDYSKDKDDELSFMEGAIIYVIKKNDDGWYEGVCNGVTGLFPGNYVESI 54
SH3_CD2AP-like_1 cd11873
First Src Homology 3 domain (SH3A) of CD2-associated protein and similar proteins; This ...
1084-1133 5.56e-09

First Src Homology 3 domain (SH3A) of CD2-associated protein and similar proteins; This subfamily is composed of the first SH3 domain (SH3A) of CD2AP, CIN85 (Cbl-interacting protein of 85 kDa), and similar domains. CD2AP and CIN85 are adaptor proteins that bind to protein partners and assemble complexes that have been implicated in T cell activation, kidney function, and apoptosis of neuronal cells. They also associate with endocytic proteins, actin cytoskeleton components, and other adaptor proteins involved in receptor tyrosine kinase (RTK) signaling. CD2AP and the main isoform of CIN85 contain three SH3 domains, a proline-rich region, and a C-terminal coiled-coil domain. All of these domains enable CD2AP and CIN85 to bind various protein partners and assemble complexes that have been implicated in many different functions. SH3A of both proteins bind to an atypical PXXXPR motif at the C-terminus of Cbl and the cytoplasmic domain of the cell adhesion protein CD2. CIN85 SH3A binds to internal proline-rich motifs within the proline-rich region; this intramolecular interaction serves as a regulatory mechanism to keep CIN85 in a closed conformation, preventing the recruitment of other proteins. CIN85 SH3A has also been shown to bind ubiquitin. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212806 [Multi-domain]  Cd Length: 53  Bit Score: 53.04  E-value: 5.56e-09
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11873      4 VEFDYDAEEPDELTLKVGDIITNVKKMEEGWWEGTLNGKRGMFPDNFVKV 53
SH3_Nebulin_family_C cd11789
C-terminal Src Homology 3 domain of the Nebulin family of proteins; Nebulin family proteins ...
1081-1133 6.17e-09

C-terminal Src Homology 3 domain of the Nebulin family of proteins; Nebulin family proteins contain multiple nebulin repeats, and may contain an N-terminal LIM domain and/or a C-terminal SH3 domain. They have molecular weights ranging from 34 to 900 kD, depending on the number of nebulin repeats, and they all bind actin. They are involved in the regulation of actin filament architecture and function as stabilizers and scaffolds for cytoskeletal structures with which they associate, such as long actin filaments or focal adhesions. Nebulin family proteins that contain a C-terminal SH3 domain include the giant filamentous protein nebulin, nebulette, Lasp1, and Lasp2. Lasp2, also called LIM-nebulette, is an alternatively spliced variant of nebulette. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212723 [Multi-domain]  Cd Length: 55  Bit Score: 53.09  E-value: 6.17e-09
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLH--GQEGLFPGNYVEK 1133
Cdd:cd11789      1 RYRAMYDYAAADDDEVSFQEGDVIINVEIIDDGWMEGTVQrtGQSGMLPANYVEL 55
SH3_Tks4_2 cd12076
Second Src homology 3 domain of Tyrosine kinase substrate with four SH3 domains; Tks4, also ...
1084-1133 6.98e-09

Second Src homology 3 domain of Tyrosine kinase substrate with four SH3 domains; Tks4, also called SH3 and PX domain-containing protein 2B (SH3PXD2B) or HOFI, is a Src substrate and scaffolding protein that plays an important role in the formation of podosomes and invadopodia, the dynamic actin-rich structures that are related to cell migration and cancer cell invasion. It is required in the formation of functional podosomes, EGF-induced membrane ruffling, and lamellipodia generation. It plays an important role in cellular attachment and cell spreading. Tks4 is essential for the localization of MT1-MMP (membrane-type 1 matrix metalloproteinase) to invadopodia. It contains an N-terminal Phox homology (PX) domain and four SH3 domains. This model characterizes the second SH3 domain of Tks4. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 213009 [Multi-domain]  Cd Length: 54  Bit Score: 52.73  E-value: 6.98e-09
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd12076      5 VIYPYTARDQDEINLEKGAVVEVIQKNLEGWWKIRYQGKEGWAPASYLKK 54
SH3_Lasp1_C cd11934
C-terminal Src Homology 3 domain of LIM and SH3 domain protein 1; Lasp1 is a cytoplasmic ...
1079-1134 9.79e-09

C-terminal Src Homology 3 domain of LIM and SH3 domain protein 1; Lasp1 is a cytoplasmic protein that binds focal adhesion proteins and is involved in cell signaling, migration, and proliferation. It is overexpressed in several cancer cells including breast, ovarian, bladder, and liver. In cancer cells, it can be found in the nucleus; its degree of nuclear localization correlates with tumor size and poor prognosis. Lasp1 is a 36kD protein containing an N-terminal LIM domain, two nebulin repeats, and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212867 [Multi-domain]  Cd Length: 59  Bit Score: 52.69  E-value: 9.79e-09
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gi 1622892340 1079 GPRCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLH--GQEGLFPGNYVEKI 1134
Cdd:cd11934      2 GKRYRAVYDYNAADEDEVSFQDGDTIVNVQQIDDGWMYGTVErtGDTGMLPANYVEAI 59
SH3_FCHSD2_2 cd11894
Second Src Homology 3 domain of FCH and double SH3 domains protein 2; FCHSD2 has a domain ...
1083-1132 9.91e-09

Second Src Homology 3 domain of FCH and double SH3 domains protein 2; FCHSD2 has a domain structure consisting of an N-terminal F-BAR (FES-CIP4 Homology and Bin/Amphiphysin/Rvs), two SH3, and C-terminal proline-rich domains. It has only been characterized in silico and its function is unknown. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212827  Cd Length: 56  Bit Score: 52.63  E-value: 9.91e-09
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEIL---MEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11894      3 KALYDYEGQTDDELSFPEGAIIRILnkeNQDDDGFWEGEFNGRIGVFPSVLVE 55
SH3_Bzz1_1 cd11912
First Src Homology 3 domain of Bzz1 and similar domains; Bzz1 (or Bzz1p) is a WASP ...
1083-1132 1.07e-08

First Src Homology 3 domain of Bzz1 and similar domains; Bzz1 (or Bzz1p) is a WASP/Las17-interacting protein involved in endocytosis and trafficking to the vacuole. It physically interacts with type I myosins and functions in the early steps of endocytosis. Together with other proteins, it induces membrane scission in yeast. Bzz1 contains an N-terminal F-BAR (FES-CIP4 Homology and Bin/Amphiphysin/Rvs), a central coiled-coil, and two C-terminal SH3 domains. This model represents the first C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212845 [Multi-domain]  Cd Length: 55  Bit Score: 52.23  E-value: 1.07e-08
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDS-SGWWKGRL-HGQEGLFPGNYVE 1132
Cdd:cd11912      3 KVLYDYTASGDDEVSISEGEEVTVLEPDDgSGWTKVRNgSGEEGLVPTSYIE 54
SH3_MLK cd11876
Src Homology 3 domain of Mixed Lineage Kinases; MLKs are Serine/Threonine Kinases (STKs), ...
1082-1131 1.16e-08

Src Homology 3 domain of Mixed Lineage Kinases; MLKs are Serine/Threonine Kinases (STKs), catalyzing the transfer of the gamma-phosphoryl group from ATP to S/T residues on protein substrates. MLKs act as mitogen-activated protein kinase kinase kinases (MAP3Ks, MKKKs, MAPKKKs), which phosphorylate and activate MAPK kinases (MAPKKs or MKKs or MAP2Ks), which in turn phosphorylate and activate MAPKs during signaling cascades that are important in mediating cellular responses to extracellular signals. MLKs play roles in immunity and inflammation, as well as in cell death, proliferation, and cell cycle regulation. Mammals have four MLKs (MLK1-4), mostly conserved in vertebrates, which contain an SH3 domain, a catalytic kinase domain, a leucine zipper, a proline-rich region, and a CRIB domain that mediates binding to GTP-bound Cdc42 and Rac. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212809 [Multi-domain]  Cd Length: 58  Bit Score: 52.52  E-value: 1.16e-08
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gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMEDSS-----GWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11876      2 WTALFDYDARGEDELTLRRGQPVEVLSKDAAvsgdeGWWTGKIGDKVGIFPSNYV 56
SH3_Eve1_3 cd11816
Third Src homology 3 domain of ADAM-binding protein Eve-1; Eve-1, also called SH3 ...
1081-1131 1.19e-08

Third Src homology 3 domain of ADAM-binding protein Eve-1; Eve-1, also called SH3 domain-containing protein 19 (SH3D19) or EEN-binding protein (EBP), exists in multiple alternatively spliced isoforms. The longest isoform contains five SH3 domain in the C-terminal region and seven proline-rich motifs in the N-terminal region. It is abundantly expressed in skeletal muscle and heart, and may be involved in regulating the activity of ADAMs (A disintegrin and metalloproteases). Eve-1 interacts with EEN, an endophilin involved in endocytosis and may be the target of the MLL-EEN fusion protein that is implicated in leukemogenesis. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212750 [Multi-domain]  Cd Length: 51  Bit Score: 52.02  E-value: 1.19e-08
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11816      1 RCVARFDFEGEQEDELSFSEGDVITLKEYVGEEWAKGELNGKIGIFPLNFV 51
SH3_Sorbs_1 cd11781
First Src Homology 3 domain of Sorbin and SH3 domain containing (Sorbs) proteins and similar ...
1082-1132 1.39e-08

First Src Homology 3 domain of Sorbin and SH3 domain containing (Sorbs) proteins and similar domains; This family, also called the vinexin family, is composed predominantly of adaptor proteins containing one sorbin homology (SoHo) and three SH3 domains. Members include the first SH3 domains of Sorbs1 (or ponsin), Sorbs2 (or ArgBP2), Vinexin (or Sorbs3), and similar domains. They are involved in the regulation of cytoskeletal organization, cell adhesion, and growth factor signaling. Members of this family bind multiple partners including signaling molecules like c-Abl, c-Arg, Sos, and c-Cbl, as well as cytoskeletal molecules such as vinculin and afadin. They may have overlapping functions. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212715 [Multi-domain]  Cd Length: 53  Bit Score: 51.96  E-value: 1.39e-08
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gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11781      2 ARALYPFKAQSAKELSLKKGDIIYIRRQIDKNWYEGEHNGRVGIFPASYVE 52
SH3_Nck_3 cd11767
Third Src Homology 3 domain of Nck adaptor proteins; This group contains the third SH3 domain ...
1083-1132 1.50e-08

Third Src Homology 3 domain of Nck adaptor proteins; This group contains the third SH3 domain of Nck, the first SH3 domain of Caenorhabditis elegans Ced-2 (Cell death abnormality protein 2), and similar domains. Nck adaptor proteins regulate actin cytoskeleton dynamics by linking proline-rich effector molecules to protein tyrosine kinases and phosphorylated signaling intermediates. They contain three SH3 domains and a C-terminal SH2 domain. They function downstream of the PDGFbeta receptor and are involved in Rho GTPase signaling and actin dynamics. Vertebrates contain two Nck adaptor proteins: Nck1 (also called Nckalpha) and Nck2 (also called Nckbeta or Growth factor receptor-bound protein 4, Grb4), which show partly overlapping functions but also bind distinct targets. Their SH3 domains are involved in recruiting downstream effector molecules, such as the N-WASP/Arp2/3 complex, which when activated induces actin polymerization that results in the production of pedestals, or protrusions of the plasma membrane. The third SH3 domain of Nck appears to prefer ligands with a PxAPxR motif. SH3 domains are protein interaction domains that usually bind to proline-rich ligands with moderate affinity and selectivity, preferentially a PxxP motif. Ced-2 is a cell corpse engulfment protein that interacts with Ced-5 in a pathway that regulates the activation of Ced-10, a Rac small GTPase.


Pssm-ID: 212701 [Multi-domain]  Cd Length: 56  Bit Score: 51.93  E-value: 1.50e-08
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEIL--MEDSSGWWKGR-LHGQEGLFPGNYVE 1132
Cdd:cd11767      3 VALYPFTGENDEELSFEKGERLEIIekPEDDPDWWKARnALGTTGLVPRNYVE 55
SH3_GRAP_C cd11951
C-terminal Src homology 3 domain of GRB2-related adaptor protein; GRAP is a GRB-2 like adaptor ...
1083-1131 1.87e-08

C-terminal Src homology 3 domain of GRB2-related adaptor protein; GRAP is a GRB-2 like adaptor protein that is highly expressed in lymphoid tissues. It acts as a negative regulator of T cell receptor (TCR)-induced lymphocyte proliferation by downregulating the signaling to the Ras/ERK pathway. It has been identified as a regulator of TGFbeta signaling in diabetic kidney tubules and may have a role in the pathogenesis of the disease. GRAP contains an N-terminal SH3 domain, a central SH2 domain, and a C-terminal SH3 domain. The C-terminal SH3 domains (SH3c) of the related proteins, GRB2 and GRAP2, have been shown to bind to classical PxxP motif ligands, as well as to non-classical motifs. GRB2 SH3c binds Gab2 (Grb2-associated binder 2) through epitopes containing RxxK motifs, while the SH3c of GRAP2 binds to the phosphatase-like protein HD-PTP via a RxxxxK motif. SH3 domains are protein interaction domains that typically bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212884  Cd Length: 53  Bit Score: 51.72  E-value: 1.87e-08
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11951      3 QAQYDFSAEDPSQLSFRRGDIIEVLDCPDPNWWRGRISGRVGFFPRNYV 51
SH3_GRB2_like_N cd11804
N-terminal Src homology 3 domain of Growth factor receptor-bound protein 2 (GRB2) and related ...
1083-1131 2.37e-08

N-terminal Src homology 3 domain of Growth factor receptor-bound protein 2 (GRB2) and related proteins; This family includes the adaptor protein GRB2 and related proteins including Drosophila melanogaster Downstream of receptor kinase (DRK), Caenorhabditis elegans Sex muscle abnormal protein 5 (Sem-5), GRB2-related adaptor protein (GRAP), GRAP2, and similar proteins. Family members contain an N-terminal SH3 domain, a central SH2 domain, and a C-terminal SH3 domain. GRB2/Sem-5/DRK is a critical signaling molecule that regulates the Ras pathway by linking tyrosine kinases to the Ras guanine nucleotide releasing protein Sos (son of sevenless), which converts Ras to the active GTP-bound state. GRAP2 plays an important role in T cell receptor (TCR) signaling by promoting the formation of the SLP-76:LAT complex, which couples the TCR to the Ras pathway. GRAP acts as a negative regulator of T cell receptor (TCR)-induced lymphocyte proliferation by downregulating the signaling to the Ras/ERK pathway. The N-terminal SH3 domain of GRB2 binds to Sos and Sos-derived proline-rich peptides. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212738 [Multi-domain]  Cd Length: 52  Bit Score: 51.20  E-value: 2.37e-08
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEIL-MEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11804      3 VAKHDFKATAEDELSFKKGSILKVLnMEDDPNWYKAELDGKEGLIPKNYI 52
SH3_Intersectin_4 cd11839
Fourth Src homology 3 domain (or SH3D) of Intersectin; Intersectins (ITSNs) are adaptor ...
1083-1133 2.64e-08

Fourth Src homology 3 domain (or SH3D) of Intersectin; Intersectins (ITSNs) are adaptor proteins that function in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. They are essential for initiating clathrin-coated pit formation. They bind to many proteins through their multidomain structure and facilitate the assembly of multimeric complexes. Vertebrates contain two ITSN proteins, ITSN1 and ITSN2, which exist in alternatively spliced short and long isoforms. The short isoforms contain two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoforms, in addition, contain RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. ITSN1 and ITSN2 are both widely expressed, with variations depending on tissue type and stage of development. The fourth SH3 domain (or SH3D) of ITSN1 has been shown to bind SHIP2, Numb, CdGAP, and N-WASP. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212773 [Multi-domain]  Cd Length: 58  Bit Score: 51.18  E-value: 2.64e-08
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHG-----QEGLFPGNYVEK 1133
Cdd:cd11839      3 QVIAPFTATAENQLSLAVGQLVLVRKKSPSGWWEGELQArgkkrQIGWFPANYVKL 58
SH3_Eve1_5 cd11818
Fifth Src homology 3 domain of ADAM-binding protein Eve-1; Eve-1, also called SH3 ...
1081-1130 2.72e-08

Fifth Src homology 3 domain of ADAM-binding protein Eve-1; Eve-1, also called SH3 domain-containing protein 19 (SH3D19) or EEN-binding protein (EBP), exists in multiple alternatively spliced isoforms. The longest isoform contains five SH3 domain in the C-terminal region and seven proline-rich motifs in the N-terminal region. It is abundantly expressed in skeletal muscle and heart, and may be involved in regulating the activity of ADAMs (A disintegrin and metalloproteases). Eve-1 interacts with EEN, an endophilin involved in endocytosis and may be the target of the MLL-EEN fusion protein that is implicated in leukemogenesis. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212752 [Multi-domain]  Cd Length: 50  Bit Score: 50.94  E-value: 2.72e-08
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNY 1130
Cdd:cd11818      1 KARALYDFTGENEDELSFKAGDIITELESIDEEWMSGELRGKSGIFPKNF 50
SH3_CRK_N cd11758
N-terminal Src Homology 3 domain of Ct10 Regulator of Kinase adaptor proteins; CRK adaptor ...
1083-1133 3.13e-08

N-terminal Src Homology 3 domain of Ct10 Regulator of Kinase adaptor proteins; CRK adaptor proteins consists of SH2 and SH3 domains, which bind tyrosine-phosphorylated peptides and proline-rich motifs, respectively. They function downstream of protein tyrosine kinases in many signaling pathways started by various extracellular signals, including growth and differentiation factors. Cellular CRK (c-CRK) contains a single SH2 domain, followed by N-terminal and C-terminal SH3 domains. It is involved in the regulation of many cellular processes including cell growth, motility, adhesion, and apoptosis. CRK has been implicated in the malignancy of various human cancers. The N-terminal SH3 domain of CRK binds a number of target proteins including DOCK180, C3G, SOS, and cABL. The CRK family includes two alternatively spliced protein forms, CRKI and CRKII, that are expressed by the CRK gene, and the CRK-like (CRKL) protein, which is expressed by a distinct gene (CRKL). SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212692 [Multi-domain]  Cd Length: 55  Bit Score: 50.82  E-value: 3.13e-08
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGR-LHGQEGLFPGNYVEK 1133
Cdd:cd11758      4 RALFDFPGNDDEDLPFKKGEILTVIRKPEEQWWNARnSEGKTGMIPVPYVEK 55
SH3_PLCgamma2 cd11969
Src homology 3 domain of Phospholipase C (PLC) gamma 2; PLCgamma2 is primarily expressed in ...
1083-1134 3.16e-08

Src homology 3 domain of Phospholipase C (PLC) gamma 2; PLCgamma2 is primarily expressed in haematopoietic cells, specifically in B cells. It is activated by tyrosine phosphorylation by B cell receptor (BCR) kinases and is recruited to the plasma membrane where its substrate is located. It is required in pre-BCR signaling and in the maturation of B cells. PLCs catalyze the hydrolysis of phosphatidylinositol (4,5)-bisphosphate [PtdIns(4,5)P2] to produce Ins(1,4,5)P3 and diacylglycerol (DAG). Ins(1,4,5)P3 initiates the calcium signaling cascade while DAG functions as an activator of PKC. PLCgamma contains a Pleckstrin homology (PH) domain followed by an elongation factor (EF) domain, two catalytic regions of PLC domains that flank two tandem SH2 domains, followed by a SH3 domain and C2 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212902  Cd Length: 55  Bit Score: 50.99  E-value: 3.16e-08
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQ-EGLFPGNYVEKI 1134
Cdd:cd11969      3 KALYDYRAKRSDELSFCKGALIHNVSKETGGWWKGDYGGKvQHYFPSNYVEDV 55
SH3_GAS7 cd11829
Src homology 3 domain of Growth Arrest Specific protein 7; GAS7 is mainly expressed in the ...
1081-1131 3.24e-08

Src homology 3 domain of Growth Arrest Specific protein 7; GAS7 is mainly expressed in the brain and is required for neurite outgrowth. It may also play a role in the protection and migration of embryonic stem cells. Treatment-related acute myeloid leukemia (AML) has been reported resulting from mixed-lineage leukemia (MLL)-GAS7 translocations as a complication of primary cancer treatment. GAS7 contains an N-terminal SH3 domain, followed by a WW domain, and a central F-BAR domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212763 [Multi-domain]  Cd Length: 52  Bit Score: 50.98  E-value: 3.24e-08
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gi 1622892340 1081 RCRALYQYVGQDVDE-LSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11829      1 LCRTLYAFTGEQHQQgLSFEAGELIRVLQAPDGGWWEGEKDGLRGWFPASYV 52
SH3_Intersectin_3 cd11838
Third Src homology 3 domain (or SH3C) of Intersectin; Intersectins (ITSNs) are adaptor ...
1084-1133 3.75e-08

Third Src homology 3 domain (or SH3C) of Intersectin; Intersectins (ITSNs) are adaptor proteins that function in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. They are essential for initiating clathrin-coated pit formation. They bind to many proteins through their multidomain structure and facilitate the assembly of multimeric complexes. Vertebrates contain two ITSN proteins, ITSN1 and ITSN2, which exist in alternatively spliced short and long isoforms. The short isoforms contain two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoforms, in addition, contain RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. ITSN1 and ITSN2 are both widely expressed, with variations depending on tissue type and stage of development. The third SH3 domain (or SH3C) of ITSN1 has been shown to bind many proteins including dynamin1/2, CIN85, c-Cbl, SHIP2, Reps1, synaptojanin-1, and WNK, among others. The SH3C of ITSN2 has been shown to bind the K15 protein of Kaposi's sarcoma-associated herpesvirus. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212772 [Multi-domain]  Cd Length: 52  Bit Score: 50.49  E-value: 3.75e-08
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSgWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11838      4 ALYPYESNEPGDLTFNAGDVILVTKKDGE-WWTGTIGDRTGIFPSNYVRP 52
PHA03378 PHA03378
EBNA-3B; Provisional
947-1074 4.15e-08

EBNA-3B; Provisional


Pssm-ID: 223065 [Multi-domain]  Cd Length: 991  Bit Score: 57.77  E-value: 4.15e-08
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gi 1622892340  947 GDGLPKSSKPTRK---GMAKGRPRRSSQAPTRAAPTRAAPGPPRGMDRNGVPPSA----RGGPLPLEimsggsshrPPRG 1019
Cdd:PHA03378   732 GRARPPAAAPGRArppAAAPGRARPPAAAPGRARPPAAAPGAPTPQPPPQAPPAPqqrpRGAPTPQP---------PPQA 802
                           90       100       110       120       130
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gi 1622892340 1020 PPSTSLGASRRPRAQL-PSEHNTEFLNVPD--QGMAGMqRKRSVGQRPVPGVGRPKPQ 1074
Cdd:PHA03378   803 GPTSMQLMPRAAPGQQgPTKQILRQLLTGGvkRGRPSL-KKPAALERQAAAGPTPSPG 859
SH3_Sorbs2_1 cd11920
First Src Homology 3 domain of Sorbin and SH3 domain containing 2 (Sorbs2), also called ...
1083-1134 4.54e-08

First Src Homology 3 domain of Sorbin and SH3 domain containing 2 (Sorbs2), also called Arg-binding protein 2 (ArgBP2); Sorbs2 or ArgBP2 is an adaptor protein containing one sorbin homology (SoHo) and three SH3 domains. It regulates actin-dependent processes including cell adhesion, morphology, and migration. It is expressed in many tissues and is abundant in the heart. Like vinexin, it is found in focal adhesion where it interacts with vinculin and afadin. It also localizes in epithelial cell stress fibers and in cardiac muscle cell Z-discs. Sorbs2 has been implicated to play roles in the signaling of c-Arg, Akt, and Pyk2. Other interaction partners of Sorbs2 include c-Abl, flotillin, spectrin, dynamin 1/2, synaptojanin, PTP-PEST, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212853 [Multi-domain]  Cd Length: 55  Bit Score: 50.39  E-value: 4.54e-08
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEKI 1134
Cdd:cd11920      4 RAVYDFKAQTSKELSFKKGDTVYILRKIDQNWYEGEHHGRVGIFPISYVEKL 55
SH3_alphaPIX cd12060
Src Homology 3 domain of alpha-Pak Interactive eXchange factor; Alpha-PIX, also called Rho ...
1083-1134 4.98e-08

Src Homology 3 domain of alpha-Pak Interactive eXchange factor; Alpha-PIX, also called Rho guanine nucleotide exchange factor 6 (ARHGEF6) or Cool (Cloned out of Library)-2, activates small GTPases by exchanging bound GDP for free GTP. It acts as a GEF for both Cdc42 and Rac 1, and is localized in dendritic spines where it regulates spine morphogenesis. It controls dendritic length and spine density in the hippocampus. Mutations in the ARHGEF6 gene cause X-linked intellectual disability in humans. PIX proteins contain an N-terminal SH3 domain followed by RhoGEF (also called Dbl-homologous or DH) and Pleckstrin Homology (PH) domains, and a C-terminal leucine-zipper domain for dimerization. The SH3 domain of PIX binds to an atypical PxxxPR motif in p21-activated kinases (PAKs) with high affinity. The binding of PAKs to PIX facilitate the localization of PAKs to focal complexes and also localizes PAKs to PIX targets Cdc43 and Rac, leading to the activation of PAKs. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212993  Cd Length: 58  Bit Score: 50.39  E-value: 4.98e-08
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEKI 1134
Cdd:cd12060      5 KARFNFKQTNEDELSVCKGDIIYVTRVEEGGWWEGTLNGKTGWFPSNYVREI 56
SH3_iASPP cd11952
Src Homology 3 (SH3) domain of Inhibitor of ASPP protein (iASPP); iASPP, also called ...
1084-1130 5.99e-08

Src Homology 3 (SH3) domain of Inhibitor of ASPP protein (iASPP); iASPP, also called RelA-associated inhibitor (RAI), is an oncoprotein that inhibits the apoptotic transactivation potential of p53. It is upregulated in human breast cancers expressing wild-type p53, in acute leukemias regardless of the p53 mutation status, as well as in ovarian cancer where it is associated with poor patient outcome and chemoresistance. iASPP is also a binding partner and negative regulator of p65RelA, which promotes cell proliferation and inhibits apoptosis; p65RelA has the opposite effect on cell growth compared to the p53 family. It contains a proline-rich region, four ankyrin (ANK) repeats, and an SH3 domain at its C-terminal half. The SH3 domain and the ANK repeats of iASPP contribute to the p53 binding site; they bind to the DNA binding domain of p53. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212885 [Multi-domain]  Cd Length: 56  Bit Score: 50.31  E-value: 5.99e-08
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSG--WWKGRLHGQEGLFPGNY 1130
Cdd:cd11952      5 ALWDYSAEFPDELSFKEGDMVTVLRKDGEGtdWWWASLCGREGYVPRNY 53
SH3_MLK1-3 cd12059
Src Homology 3 domain of Mixed Lineage Kinases 1, 2, and 3; MLKs 1, 2, and 3 are Serine ...
1084-1131 7.42e-08

Src Homology 3 domain of Mixed Lineage Kinases 1, 2, and 3; MLKs 1, 2, and 3 are Serine/Threonine Kinases (STKs), catalyzing the transfer of the gamma-phosphoryl group from ATP to S/T residues on protein substrates. MLKs act as mitogen-activated protein kinase kinase kinases (MAP3Ks, MKKKs, MAPKKKs), which phosphorylate and activate MAPK kinases (MAPKKs or MKKs or MAP2Ks), which in turn phosphorylate and activate MAPKs during signaling cascades that are important in mediating cellular responses to extracellular signals. MLKs play roles in immunity and inflammation, as well as in cell death, proliferation, and cell cycle regulation. Little is known about the specific function of MLK1, also called MAP3K9. It is capable of activating the c-Jun N-terminal kinase pathway. Mice lacking both MLK1 and MLK2 are viable, fertile, and have normal life spans. MLK2, also called MAP3K10, is abundant in brain, skeletal muscle, and testis. It functions upstream of the MAPK, c-Jun N-terminal kinase. It binds hippocalcin, a calcium-sensor protein that protects neurons against calcium-induced cell death. Both MLK2 and hippocalcin may be associated with the pathogenesis of Parkinson's disease. MLK3, also called MAP3K11, is highly expressed in breast cancer cells and its signaling through c-Jun N-terminal kinase has been implicated in the migration, invasion, and malignancy of cancer cells. It also functions as a negative regulator of Inhibitor of Nuclear Factor-KappaB Kinase (IKK) and thus, impacts inflammation and immunity. MLKs contain an SH3 domain, a catalytic kinase domain, a leucine zipper, a proline-rich region, and a CRIB domain that mediates binding to GTP-bound Cdc42 and Rac. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212992 [Multi-domain]  Cd Length: 58  Bit Score: 50.15  E-value: 7.42e-08
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSS-----GWWKGRLHGQEGLFPGNYV 1131
Cdd:cd12059      4 AVFDYEASAEDELTLRRGDRVEVLSKDSAvsgdeGWWTGKINDRVGIFPSNYV 56
SH3_ASAP cd11821
Src homology 3 domain of ArfGAP with SH3 domain, ankyrin repeat and PH domain containing ...
1081-1130 7.72e-08

Src homology 3 domain of ArfGAP with SH3 domain, ankyrin repeat and PH domain containing proteins; ASAPs are Arf GTPase activating proteins (GAPs) and they function in regulating cell growth, migration, and invasion. They contain an N-terminal BAR domain, followed by a Pleckstrin homology (PH) domain, an Arf GAP domain, ankyrin (ANK) repeats, and a C-terminal SH3 domain. Vertebrates contain at least three members, ASAP1, ASAP2, and ASAP3, but some ASAP3 proteins do not seem to harbor a C-terminal SH3 domain. ASAP1 and ASAP2 show GTPase activating protein (GAP) activity towards Arf1 and Arf5. They do not show GAP activity towards Arf6, but are able to mediate Arf6 signaling by binding stably to GTP-Arf6. ASAP3 is an Arf6-specific GAP. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212755 [Multi-domain]  Cd Length: 53  Bit Score: 49.62  E-value: 7.72e-08
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQ---EGLFPGNY 1130
Cdd:cd11821      1 RVRALYDCQADNDDELTFSEGEIIVVTGEEDDEWWEGHIEGDpsrRGVFPVSF 53
SH3_ARHGEF9_like cd11828
Src homology 3 domain of ARHGEF9-like Rho guanine nucleotide exchange factors; Members of this ...
1084-1131 8.21e-08

Src homology 3 domain of ARHGEF9-like Rho guanine nucleotide exchange factors; Members of this family contain a SH3 domain followed by RhoGEF (also called Dbl-homologous or DH) and Pleckstrin Homology (PH) domains. They include the Rho guanine nucleotide exchange factors ARHGEF9, ASEF (also called ARHGEF4), ASEF2, and similar proteins. GEFs activate small GTPases by exchanging bound GDP for free GTP. ARHGEF9 specifically activates Cdc42, while both ASEF and ASEF2 can activate Rac1 and Cdc42. ARHGEF9 is highly expressed in the brain and it interacts with gephyrin, a postsynaptic protein associated with GABA and glycine receptors. ASEF plays a role in angiogenesis and cell migration. ASEF2 is important in cell migration and adhesion dynamics. ASEF exists in an autoinhibited form and is activated upon binding of the tumor suppressor APC (adenomatous polyposis coli), leading to the activation of Rac1 or Cdc42. In its autoinhibited form, the SH3 domain of ASEF forms an extensive interface with the DH and PH domains, blocking the Rac binding site. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212762 [Multi-domain]  Cd Length: 53  Bit Score: 49.69  E-value: 8.21e-08
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11828      4 ALWDHVTMDPEELGFKAGDVIEVLDMSDKDWWWGSIRDEEGWFPASFV 51
SH3_CAS cd11844
Src homology 3 domain of CAS (Crk-Associated Substrate) scaffolding proteins; CAS proteins ...
1083-1132 8.91e-08

Src homology 3 domain of CAS (Crk-Associated Substrate) scaffolding proteins; CAS proteins function as molecular scaffolds to regulate protein complexes that are involved in many cellular processes including migration, chemotaxis, apoptosis, differentiation, and progenitor cell function. They mediate the signaling of integrins at focal adhesions where they localize, and thus, regulate cell invasion and survival. Over-expression of these proteins is implicated in poor prognosis, increased metastasis, and resistance to chemotherapeutics in many cancers such as breast, lung, melanoma, and glioblastoma. CAS proteins have also been linked to the pathogenesis of inflammatory disorders, Alzheimer's, Parkinson's, and developmental defects. They share a common domain structure that includes an N-terminal SH3 domain, an unstructured substrate domain that contains many YxxP motifs, a serine-rich four-helix bundle, and a FAT-like C-terminal domain. Vertebrates contain four CAS proteins: BCAR1 (or p130Cas), NEDD9 (or HEF1), EFS (or SIN), and CASS4 (or HEPL). The SH3 domain of CAS proteins binds to diverse partners including FAK, FRNK, Pyk2, PTP-PEST, DOCK180, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212778  Cd Length: 56  Bit Score: 49.65  E-value: 8.91e-08
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSS---GWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11844      3 RALYDNVAESPDELAFRRGDILTVLEQNTAgleGWWLCSLRGRQGIAPGNRLK 55
SH3_VAV3_2 cd11978
C-terminal (or second) Src homology 3 domain of VAV3 protein; VAV3 is ubiquitously expressed ...
1084-1133 9.34e-08

C-terminal (or second) Src homology 3 domain of VAV3 protein; VAV3 is ubiquitously expressed and functions as a phosphorylation-dependent guanine nucleotide exchange factor (GEF) for RhoA, RhoG, and Rac1. It has been implicated to function in the hematopoietic, bone, cerebellar, and cardiovascular systems. VAV3 is essential in axon guidance in neurons that control blood pressure and respiration. It is overexpressed in prostate cancer cells and it plays a role in regulating androgen receptor transcriptional activity. VAV proteins contain several domains that enable their function: N-terminal calponin homology (CH), acidic, RhoGEF (also called Dbl-homologous or DH), Pleckstrin Homology (PH), C1 (zinc finger), SH2, and two SH3 domains. The SH3 domain of VAV is involved in the localization of proteins to specific sites within the cell, by interacting with proline-rich sequences within target proteins. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212911 [Multi-domain]  Cd Length: 56  Bit Score: 49.64  E-value: 9.34e-08
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSS-GWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11978      5 ARYDFCARDMRELSLLKGDVVKIYTKMSTnGWWRGEVNGRVGWFPSTYVEE 55
SH3_SGSM3 cd11813
Src Homology 3 domain of Small G protein Signaling Modulator 3; SGSM3 is also called ...
1081-1132 9.95e-08

Src Homology 3 domain of Small G protein Signaling Modulator 3; SGSM3 is also called Merlin-associated protein (MAP), RUN and SH3 domain-containing protein (RUSC3), RUN and TBC1 domain-containing protein 3 (RUTBC3), Rab GTPase-activating protein 5 (RabGAP5), or Rab GAP-like protein (RabGAPLP). It is expressed ubiquitously and functions as a regulator of small G protein RAP- and RAB-mediated neuronal signaling. It is involved in modulating NGF-mediated neurite outgrowth and differentiation. It also interacts with the tumor suppressor merlin and may play a role in the merlin-associated suppression of cell growth. SGSM3 contains TBC, SH3, and RUN domains. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212747  Cd Length: 53  Bit Score: 49.42  E-value: 9.95e-08
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11813      1 RAKALLDFERHDDDELGFRKNDIITIISQKDEHCWVGELNGLRGWFPAKFVE 52
SH3_VAV_2 cd11830
C-terminal (or second) Src homology 3 domain of VAV proteins; VAV proteins function both as ...
1084-1133 1.33e-07

C-terminal (or second) Src homology 3 domain of VAV proteins; VAV proteins function both as cytoplasmic guanine nucleotide exchange factors (GEFs) for Rho GTPases and scaffold proteins and they play important roles in cell signaling by coupling cell surface receptors to various effector functions. They play key roles in processes that require cytoskeletal reorganization including immune synapse formation, phagocytosis, cell spreading, and platelet aggregation, among others. Vertebrates have three VAV proteins (VAV1, VAV2, and VAV3). VAV proteins contain several domains that enable their function: N-terminal calponin homology (CH), acidic, RhoGEF (also called Dbl-homologous or DH), Pleckstrin Homology (PH), C1 (zinc finger), SH2, and two SH3 domains. The SH3 domain of VAV is involved in the localization of proteins to specific sites within the cell, by interacting with proline-rich sequences within target proteins. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212764 [Multi-domain]  Cd Length: 54  Bit Score: 49.17  E-value: 1.33e-07
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSS-GWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11830      4 ARYDFCARDMRELSLKEGDVVKIYNKKGQqGWWRGEINGRIGWFPSTYVEE 54
SH3_Sho1p cd11855
Src homology 3 domain of High osmolarity signaling protein Sho1p; Sho1p (or Sho1), also called ...
1081-1132 1.37e-07

Src homology 3 domain of High osmolarity signaling protein Sho1p; Sho1p (or Sho1), also called SSU81 (Suppressor of SUA8-1 mutation), is a yeast membrane protein that regulates adaptation to high salt conditions by activating the HOG (high-osmolarity glycerol) pathway. High salt concentrations lead to the localization to the membrane of the MAPKK Pbs2, which is then activated by the MAPKK Ste11 and in turn, activates the MAPK Hog1. Pbs2 is localized to the membrane though the interaction of its PxxP motif with the SH3 domain of Sho1p. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212789 [Multi-domain]  Cd Length: 55  Bit Score: 49.34  E-value: 1.37e-07
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gi 1622892340 1081 RCRALYQYVG--QDVDELSFNVNEVIEIlmEDSSG-WWKGRL-HGQEGLFPGNYVE 1132
Cdd:cd11855      1 RARALYPYDAspDDPNELSFEKGEILEV--SDTSGkWWQARKsNGETGICPSNYLQ 54
SH3_Myosin-I_fungi cd11858
Src homology 3 domain of Type I fungal Myosins; Type I myosins (myosin-I) are actin-dependent ...
1081-1132 1.51e-07

Src homology 3 domain of Type I fungal Myosins; Type I myosins (myosin-I) are actin-dependent motors in endocytic actin structures and actin patches. They play roles in membrane traffic in endocytic and secretory pathways, cell motility, and mechanosensing. Saccharomyces cerevisiae has two myosins-I, Myo3 and Myo5, which are involved in endocytosis and the polarization of the actin cytoskeleton. Myosin-I contains an N-terminal actin-activated ATPase, a phospholipid-binding TH1 (tail homology 1) domain, and a C-terminal extension which includes an F-actin-binding TH2 domain, an SH3 domain, and an acidic peptide that participates in activating the Arp2/3complex. The SH3 domain of myosin-I is required for myosin-I-induced actin polymerization. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212792 [Multi-domain]  Cd Length: 55  Bit Score: 48.92  E-value: 1.51e-07
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQ--EGLFPGNYVE 1132
Cdd:cd11858      1 TYKALYDFAGSVANELSLKKDDIVYIVQKEDNGWWLAKKLDEskEGWVPAAYLE 54
SH3_SH3RF2_1 cd11929
First Src Homology 3 domain of SH3 domain containing ring finger 2; SH3RF2 is also called ...
1080-1132 2.04e-07

First Src Homology 3 domain of SH3 domain containing ring finger 2; SH3RF2 is also called POSHER (POSH-eliminating RING protein) or HEPP1 (heart protein phosphatase 1-binding protein). It acts as an anti-apoptotic regulator of the JNK pathway by binding to and promoting the degradation of SH3RF1 (or POSH), a scaffold protein that is required for pro-apoptotic JNK activation. It may also play a role in cardiac functions together with protein phosphatase 1. SH3RF2 contains an N-terminal RING finger domain and three SH3 domains. This model represents the first SH3 domain, located at the N-terminal half, of SH3RF2. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212862  Cd Length: 54  Bit Score: 48.78  E-value: 2.04e-07
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gi 1622892340 1080 PRCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11929      1 PRAKALCNYRGHNPGDLKFNKGDVILLRRQLDENWYLGEINGVSGIFPASSVE 53
SH3_Cyk3p-like cd11889
Src Homology 3 domain of Cytokinesis protein 3 and similar proteins; Cytokinesis protein 3 ...
1081-1131 2.50e-07

Src Homology 3 domain of Cytokinesis protein 3 and similar proteins; Cytokinesis protein 3 (Cyk3 or Cyk3p) is a component of the actomyosin ring independent cytokinesis pathway in yeast. It interacts with Inn1 and facilitates its recruitment to the bud neck, thereby promoting cytokinesis. Cyk3p contains an N-terminal SH3 domain and a C-terminal transglutaminase-like domain. The Cyk3p SH3 domain binds to the C-terminal proline-rich region of Inn1. SH3 domains bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs; they play a role in the regulation of enzymes by intramolecular interactions, changing the subcellular localization of signal pathway components and mediate multiprotein complex assemblies.


Pssm-ID: 212822  Cd Length: 53  Bit Score: 48.26  E-value: 2.50e-07
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRL--HGQEGLFPGNYV 1131
Cdd:cd11889      1 KVKAVYSWAGETEGDLGFLEGDLIEVLSIGDGSWWSGKLrrNGAEGIFPSNFV 53
SH3_BCAR1 cd12001
Src homology 3 domain of the CAS (Crk-Associated Substrate) scaffolding protein family member, ...
1083-1129 2.66e-07

Src homology 3 domain of the CAS (Crk-Associated Substrate) scaffolding protein family member, Breast Cancer Anti-estrogen Resistance 1; BCAR1, also called p130cas or CASS1, is the founding member of the CAS family of scaffolding proteins and was originally identified through its ability to associate with Crk. The name BCAR1 was designated because the human gene was identified in a screen for genes that promote resistance to tamoxifen. It is widely expressed and its deletion is lethal in mice. It plays a role in regulating cell motility, survival, proliferation, transformation, cancer progression, and bacterial pathogenesis. CAS proteins function as molecular scaffolds to regulate protein complexes that are involved in many cellular processes. They share a common domain structure that includes an N-terminal SH3 domain, an unstructured substrate domain that contains many YxxP motifs, a serine-rich four-helix bundle, and a FAT-like C-terminal domain. The SH3 domain of CAS proteins binds to diverse partners including FAK, FRNK, Pyk2, PTP-PEST, DOCK180, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212934  Cd Length: 68  Bit Score: 48.88  E-value: 2.66e-07
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSG---WWKGRLHGQEGLFPGN 1129
Cdd:cd12001      6 KALYDNVAESPDELSFRKGDIMTVLERDTQGldgWWLCSLHGRQGIVPGN 55
SH3_CIP4-like cd11911
Src Homology 3 domain of Cdc42-Interacting Protein 4; This subfamily is composed of ...
1081-1132 3.23e-07

Src Homology 3 domain of Cdc42-Interacting Protein 4; This subfamily is composed of Cdc42-Interacting Protein 4 (CIP4), Formin Binding Protein 17 (FBP17), FormiN Binding Protein 1-Like (FNBP1L), and similar proteins. CIP4 and FNBP1L are Cdc42 effectors that bind Wiskott-Aldrich syndrome protein (WASP) and function in endocytosis. CIP4 and FBP17 bind to the Fas ligand and may be implicated in the inflammatory response. CIP4 may also play a role in phagocytosis. It functions downstream of Cdc42 in PDGF-dependent actin reorganization and cell migration, and also regulates the activity of PDGFRbeta. It uses Src as a substrate in regulating the invasiveness of breast tumor cells. CIP4 may also play a role in the pathogenesis of Huntington's disease. Members of this subfamily typically contain an N-terminal F-BAR (FES-CIP4 Homology and Bin/Amphiphysin/Rvs) domain, a central Cdc42-binding HR1 domain, and a C-terminal SH3 domain. The SH3 domain of CIP4 associates with Gapex-5, a Rab31 GEF. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212844 [Multi-domain]  Cd Length: 55  Bit Score: 48.02  E-value: 3.23e-07
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDS-SGWWKGRL-HGQEGLFPGNYVE 1132
Cdd:cd11911      1 TCTALYDFDGTSEGTLSMEEGEILLVLEEDGgDGWTRVRKnNGDEGYVPTSYIE 54
SH3_GRAP2_N cd11947
N-terminal Src homology 3 domain of GRB2-related adaptor protein 2; GRAP2 is also called GADS ...
1083-1132 3.64e-07

N-terminal Src homology 3 domain of GRB2-related adaptor protein 2; GRAP2 is also called GADS (GRB2-related adapter downstream of Shc), GrpL, GRB2L, Mona, or GRID (Grb2-related protein with insert domain). It is expressed specifically in the hematopoietic system. It plays an important role in T cell receptor (TCR) signaling by promoting the formation of the SLP-76:LAT complex, which couples the TCR to the Ras pathway. It also have roles in antigen-receptor and tyrosine kinase mediated signaling. GRAP2 is unique from other GRB2-like adaptor proteins in that it can be regulated by caspase cleavage. It contains an N-terminal SH3 domain, a central SH2 domain, and a C-terminal SH3 domain. The N-terminal SH3 domain of the related protein GRB2 binds to Sos and Sos-derived proline-rich peptides. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212880 [Multi-domain]  Cd Length: 52  Bit Score: 47.87  E-value: 3.64e-07
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSgWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11947      3 RGKFDFTASGEDELSFKKGDVLKILSSDDI-WFKAELNGEEGYVPKNFVD 51
SH3_UBASH3 cd11791
Src homology 3 domain of Ubiquitin-associated and SH3 domain-containing proteins, also called ...
1082-1133 4.32e-07

Src homology 3 domain of Ubiquitin-associated and SH3 domain-containing proteins, also called TULA (T cell Ubiquitin LigAnd) family of proteins; UBASH3 or TULA proteins are also referred to as Suppressor of T cell receptor Signaling (STS) proteins. They contain an N-terminal UBA domain, a central SH3 domain, and a C-terminal histidine phosphatase domain. They bind c-Cbl through the SH3 domain and to ubiquitin via UBA. In some vertebrates, there are two TULA family proteins, called UBASH3A (also called TULA or STS-2) and UBASH3B (also called TULA-2 or STS-1), which show partly overlapping as well as distinct functions. UBASH3B is widely expressed while UBASH3A is only found in lymphoid cells. UBASH3A facilitates apoptosis induced in T cells through its interaction with the apoptosis-inducing factor AIF. UBASH3B is an active phosphatase while UBASH3A is not. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212725 [Multi-domain]  Cd Length: 59  Bit Score: 48.07  E-value: 4.32e-07
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gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVI----EILMEDSSGWWKGRLH--GQEGLFPGNYVEK 1133
Cdd:cd11791      2 LRVLYPYTPQEEDELELVPGDYIyvspEELDSSSDGWVEGTSWltGCSGLLPENYTEK 59
SH3_srGAP cd11809
Src homology 3 domain of Slit-Robo GTPase Activating Proteins; Slit-Robo GTPase Activating ...
1084-1131 4.33e-07

Src homology 3 domain of Slit-Robo GTPase Activating Proteins; Slit-Robo GTPase Activating Proteins (srGAPs) are Rho GAPs that interact with Robo1, the transmembrane receptor of Slit proteins. Slit proteins are secreted proteins that control axon guidance and the migration of neurons and leukocytes. Vertebrates contain three isoforms of srGAPs (srGAP1-3), all of which are expressed during embryonic and early development in the nervous system but with different localization and timing. A fourth member has also been reported (srGAP4, also called ARHGAP4). srGAPs contain an N-terminal F-BAR domain, a Rho GAP domain, and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212743 [Multi-domain]  Cd Length: 53  Bit Score: 47.78  E-value: 4.33e-07
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11809      4 AQFDYTGRSERELSFKKGDSLTLYRQVSDDWWRGQLNGQDGLVPHKYI 51
SH3_CSK cd11769
Src Homology 3 domain of C-terminal Src kinase; CSK is a cytoplasmic (or nonreceptor) tyr ...
1079-1133 4.52e-07

Src Homology 3 domain of C-terminal Src kinase; CSK is a cytoplasmic (or nonreceptor) tyr kinase containing the Src homology domains, SH3 and SH2, N-terminal to the catalytic tyr kinase domain. They negatively regulate the activity of Src kinases that are anchored to the plasma membrane. To inhibit Src kinases, CSK is translocated to the membrane via binding to specific transmembrane proteins, G-proteins, or adaptor proteins near the membrane. CSK catalyzes the tyr phosphorylation of the regulatory C-terminal tail of Src kinases, resulting in their inactivation. It is expressed in a wide variety of tissues and plays a role, as a regulator of Src, in cell proliferation, survival, and differentiation, and consequently, in cancer development and progression. In addition, CSK also shows Src-independent functions. It is a critical component in G-protein signaling, and plays a role in cytoskeletal reorganization and cell migration. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212703 [Multi-domain]  Cd Length: 57  Bit Score: 47.68  E-value: 4.52e-07
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*...
gi 1622892340 1079 GPRCRALYQYVGQDVDELSFNVNEVIEIL--MEDSSgWWKGR-LHGQEGLFPGNYVEK 1133
Cdd:cd11769      1 GTECIAKYNFNGASEEDLPFKKGDILTIVavTKDPN-WYKAKnKDGREGMIPANYVQK 57
SH3_FCHSD1_2 cd11895
Second Src Homology 3 domain of FCH and double SH3 domains protein 1; FCHSD1 has a domain ...
1083-1134 4.82e-07

Second Src Homology 3 domain of FCH and double SH3 domains protein 1; FCHSD1 has a domain structure consisting of an N-terminal F-BAR (FES-CIP4 Homology and Bin/Amphiphysin/Rvs), two SH3, and C-terminal proline-rich domains. It has only been characterized in silico and its function is unknown. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212828  Cd Length: 58  Bit Score: 47.65  E-value: 4.82e-07
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*.
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEIL--MEDS--SGWWKGRLHGQEGLFPGNYVEKI 1134
Cdd:cd11895      3 RALYSYTGQSPEELSFPEGALIRLLprAQDGvdDGFWRGEFGGRVGVFPSLLVEEL 58
SH3_Nebulette_C cd11935
C-terminal Src Homology 3 domain of Nebulette and LIM-nebulette (or Lasp2); Nebulette is a ...
1083-1134 5.65e-07

C-terminal Src Homology 3 domain of Nebulette and LIM-nebulette (or Lasp2); Nebulette is a cardiac-specific protein that localizes to the Z-disc. It interacts with tropomyosin and is important in stabilizing actin thin filaments in cardiac muscles. Polymorphisms in the nebulette gene are associated with dilated cardiomyopathy, with some mutations resulting in severe heart failure. Nebulette is a 107kD protein that contains an N-terminal acidic region, multiple nebulin repeats, and a C-terminal SH3 domain. LIM-nebulette, also called Lasp2 (LIM and SH3 domain protein 2), is an alternatively spliced variant of nebulette. Although it shares a gene with nebulette, Lasp2 is not transcribed from a muscle-specific promoter, giving rise to its multiple tissue expression pattern with highest amounts in the brain. It can crosslink actin filaments and it affects cell spreading. Lasp2 is a 34kD protein containing an N-terminal LIM domain, three nebulin repeats, and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212868 [Multi-domain]  Cd Length: 58  Bit Score: 47.69  E-value: 5.65e-07
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLH--GQEGLFPGNYVEKI 1134
Cdd:cd11935      4 RAMYDYSAQDEDEVSFRDGDYIVNVQPIDEGWMYGTVQrtGRTGMLPANYIEFV 57
SH3_Sla1p_1 cd11773
First Src Homology 3 domain of the fungal endocytic adaptor protein Sla1p; Sla1p facilitates ...
1082-1130 5.97e-07

First Src Homology 3 domain of the fungal endocytic adaptor protein Sla1p; Sla1p facilitates endocytosis by playing a role as an adaptor protein in coupling components of the actin cytoskeleton to the endocytic machinery. It interacts with Abp1p, Las17p and Pan1p, which are activator proteins of actin-related protein 2/3 (Arp2/3). Sla1p contains multiple domains including three SH3 domains, a SAM (sterile alpha motif) domain, and a Sla1 homology domain 1 (SHD1), which binds to the NPFXD motif that is found in many integral membrane proteins such as the Golgi-localized Arf-binding protein Lsb5p and the P4-ATPases, Drs2p and Dnf1p. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212707 [Multi-domain]  Cd Length: 57  Bit Score: 47.42  E-value: 5.97e-07
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*.
gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLH-------GQEGLFPGNY 1130
Cdd:cd11773      2 YKALYDYEPQTEDELTIQEDDILYLLEKSDDDWWKVKLKvnssdddEPVGLVPATY 57
SH3_ASPP cd11807
Src homology 3 domain of Apoptosis Stimulating of p53 proteins (ASPP); The ASPP family of ...
1084-1130 6.60e-07

Src homology 3 domain of Apoptosis Stimulating of p53 proteins (ASPP); The ASPP family of proteins bind to important regulators of apoptosis (p53, Bcl-2, and RelA) and cell growth (APCL, PP1). They share similarity at their C-termini, where they harbor a proline-rich region, four ankyrin (ANK) repeats, and an SH3 domain. Vertebrates contain three members of the family: ASPP1, ASPP2, and iASPP. ASPP1 and ASPP2 activate the apoptotic function of the p53 family of tumor suppressors (p53, p63, and p73), while iASPP is an oncoprotein that specifically inhibits p53-induced apoptosis. The expression of ASPP proteins is altered in tumors; ASPP1 and ASPP2 are downregulated whereas iASPP is upregulated is some cancer types. ASPP proteins also bind and regulate protein phosphatase 1 (PP1), and this binding is competitive with p53 binding. The SH3 domain and the ANK repeats of ASPP contribute to the p53 binding site; they bind to the DNA binding domain of p53. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212741 [Multi-domain]  Cd Length: 57  Bit Score: 47.37  E-value: 6.60e-07
                           10        20        30        40        50
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILM---EDSSGWWKGRLHGQEGLFPGNY 1130
Cdd:cd11807      5 ALFDYEAENGDELSFREGDELTVLRkgdDDETEWWWARLNDKEGYVPRNL 54
SH3_SH3RF3_1 cd11928
First Src Homology 3 domain of SH3 domain containing ring finger 3, an E3 ubiquitin-protein ...
1080-1132 7.17e-07

First Src Homology 3 domain of SH3 domain containing ring finger 3, an E3 ubiquitin-protein ligase; SH3RF3 is also called POSH2 (Plenty of SH3s 2) or SH3MD4 (SH3 multiple domains protein 4). It is a scaffold protein with E3 ubiquitin-protein ligase activity. It was identified in the screen for interacting partners of p21-activated kinase 2 (PAK2). It may play a role in regulating JNK mediated apoptosis in certain conditions. It also interacts with GTP-loaded Rac1. SH3RF3 is highly homologous to SH3RF1; it also contains an N-terminal RING finger domain and four SH3 domains. This model represents the first SH3 domain, located at the N-terminal half, of SH3RF3. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212861  Cd Length: 54  Bit Score: 47.22  E-value: 7.17e-07
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1080 PRCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11928      1 PCGKALYSYEGKEPGDLKFNKGDIIILRRKVDENWYHGELNGCHGFLPASYIQ 53
SH3_NEDD9 cd12002
Src homology 3 domain of CAS (Crk-Associated Substrate) scaffolding protein family member, ...
1083-1132 7.86e-07

Src homology 3 domain of CAS (Crk-Associated Substrate) scaffolding protein family member, Neural precursor cell Expressed, Developmentally Down-regulated 9; NEDD9 is also called human enhancer of filamentation 1 (HEF1) or CAS-L (Crk-associated substrate in lymphocyte). It was first described as a gene predominantly expressed in early embryonic brain, and was also isolated from a screen of human proteins that regulate filamentous budding in yeast, and as a tyrosine phosphorylated protein in lymphocytes. It promotes metastasis in different solid tumors. NEDD9 localizes in focal adhesions and associates with FAK and Abl kinase. It also interacts with SMAD3 and the proteasomal machinery which allows its rapid turnover; these interactions are not shared by other CAS proteins. CAS proteins function as molecular scaffolds to regulate protein complexes that are involved in many cellular processes. They share a common domain structure that includes an N-terminal SH3 domain, an unstructured substrate domain that contains many YxxP motifs, a serine-rich four-helix bundle, and a FAT-like C-terminal domain. The SH3 domain of CAS proteins binds to diverse partners including FAK, FRNK, Pyk2, PTP-PEST, DOCK180, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212935  Cd Length: 57  Bit Score: 47.29  E-value: 7.86e-07
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDS---SGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd12002      3 RALYDNVPECAEELAFRKGDILTVIEQNTgglEGWWLCSLHGRQGIAPGNRLK 55
SH3_Intersectin2_2 cd11990
Second Src homology 3 domain (or SH3B) of Intersectin-2; Intersectin-2 (ITSN2) is an adaptor ...
1081-1132 8.10e-07

Second Src homology 3 domain (or SH3B) of Intersectin-2; Intersectin-2 (ITSN2) is an adaptor protein that functions in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. It plays a role in clathrin-coated pit (CCP) formation. It binds to many proteins through its multidomain structure and facilitate the assembly of multimeric complexes. ITSN2 also functions as a specific GEF for Cdc42 activation in epithelial morphogenesis, and is required in mitotic spindle orientation. It exists in alternatively spliced short and long isoforms. The short isoform contains two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoform, in addition, contains RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. The second SH3 domain (or SH3B) of ITSN2 is expected to bind protein partners, similar to ITSN1 which has been shown to bind WNK and CdGAP. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212923 [Multi-domain]  Cd Length: 52  Bit Score: 46.96  E-value: 8.10e-07
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|..
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILmEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11990      1 KAQALCSWTAKKDNHLNFSKNDIITVL-EQQENWWFGEVHGGRGWFPKSYVK 51
SH3_Amphiphysin cd11790
Src Homology 3 domain of Amphiphysin and related domains; Amphiphysins function primarily in ...
1081-1134 9.05e-07

Src Homology 3 domain of Amphiphysin and related domains; Amphiphysins function primarily in endocytosis and other membrane remodeling events. They exist in several isoforms and mammals possess two amphiphysin proteins from distinct genes. Amphiphysin I proteins, enriched in the brain and nervous system, contain domains that bind clathrin, Adaptor Protein complex 2 (AP2), dynamin, and synaptojanin. They function in synaptic vesicle endocytosis. Human autoantibodies to amphiphysin I hinder GABAergic signaling and contribute to the pathogenesis of paraneoplastic stiff-person syndrome. Some amphiphysin II isoforms, also called Bridging integrator 1 (Bin1), are localized in many different tissues and may function in intracellular vesicle trafficking. In skeletal muscle, Bin1 plays a role in the organization and maintenance of the T-tubule network. Mutations in Bin1 are associated with autosomal recessive centronuclear myopathy. Amphiphysins contain an N-terminal BAR domain with an additional N-terminal amphipathic helix (an N-BAR), a variable central domain, and a C-terminal SH3 domain. The SH3 domain of amphiphysins bind proline-rich motifs present in binding partners such as dynamin, synaptojanin, and nsP3. It also belongs to a subset of SH3 domains that bind ubiquitin in a site that overlaps with the peptide binding site. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212724 [Multi-domain]  Cd Length: 64  Bit Score: 47.32  E-value: 9.05e-07
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEIL-----MEDSSGWWKGRLH--GQEGLFPGNYVEKI 1134
Cdd:cd11790      4 KVRATHDYTAEDTDELTFEKGDVILVIpfddpEEQDEGWLMGVKEstGCRGVFPENFTERI 64
SH3_Sorbs_2 cd11782
Second Src Homology 3 domain of Sorbin and SH3 domain containing (Sorbs) proteins and similar ...
1083-1132 9.18e-07

Second Src Homology 3 domain of Sorbin and SH3 domain containing (Sorbs) proteins and similar domains; This family, also called the vinexin family, is composed predominantly of adaptor proteins containing one sorbin homology (SoHo) and three SH3 domains. Members include the second SH3 domains of Sorbs1 (or ponsin), Sorbs2 (or ArgBP2), Vinexin (or Sorbs3), and similar domains. They are involved in the regulation of cytoskeletal organization, cell adhesion, and growth factor signaling. Members of this family bind multiple partners including signaling molecules like c-Abl, c-Arg, Sos, and c-Cbl, as well as cytoskeletal molecules such as vinculin and afadin. They may have overlapping functions. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212716 [Multi-domain]  Cd Length: 53  Bit Score: 46.96  E-value: 9.18e-07
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11782      3 RAKYNFNADTGVELSFRKGDVITLTRRVDENWYEGRIGGRQGIFPVSYVQ 52
SH3_ASEF2 cd11974
Src homology 3 domain of APC-Stimulated guanine nucleotide Exchange Factor 2; ASEF2, also ...
1084-1131 1.07e-06

Src homology 3 domain of APC-Stimulated guanine nucleotide Exchange Factor 2; ASEF2, also called Spermatogenesis-associated protein 13 (SPATA13), is a GEF that localizes with actin at the leading edge of cells and is important in cell migration and adhesion dynamics. GEFs activate small GTPases by exchanging bound GDP for free GTP. ASEF2 can activate both Rac 1 and Cdc42, but only Rac1 activation is necessary for increased cell migration and adhesion turnover. Together with APC (adenomatous polyposis coli) and Neurabin2, a scaffold protein that binds F-actin, it is involved in regulating HGF-induced cell migration. ASEF2 contains a SH3 domain followed by RhoGEF (also called Dbl-homologous or DH) and Pleckstrin Homology (PH) domains. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212907  Cd Length: 54  Bit Score: 46.60  E-value: 1.07e-06
                           10        20        30        40
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11974      5 ALWDHVTMDDQELAFKAGDVIRVLEASNKDWWWGRNEDREAWFPASFV 52
SH3_Sorbs_3 cd11780
Third (or C-terminal) Src Homology 3 domain of Sorbin and SH3 domain containing (Sorbs) ...
1081-1133 1.08e-06

Third (or C-terminal) Src Homology 3 domain of Sorbin and SH3 domain containing (Sorbs) proteins and similar domains; This family, also called the vinexin family, is composed predominantly of adaptor proteins containing one sorbin homology (SoHo) and three SH3 domains. Members include the third SH3 domains of Sorbs1 (or ponsin), Sorbs2 (or ArgBP2), Vinexin (or Sorbs3), and similar domains. They are involved in the regulation of cytoskeletal organization, cell adhesion, and growth factor signaling. Members of this family bind multiple partners including signaling molecules like c-Abl, c-Arg, Sos, and c-Cbl, as well as cytoskeletal molecules such as vinculin and afadin. They may have overlapping functions. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212714 [Multi-domain]  Cd Length: 55  Bit Score: 46.53  E-value: 1.08e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKG--RLHGQEGLFPGNYVEK 1133
Cdd:cd11780      1 RYRALYSYTPQNEDELELREGDIVYVMEKCDDGWFVGtsERTGLFGTFPGNYVAR 55
PHA03378 PHA03378
EBNA-3B; Provisional
955-1080 1.19e-06

EBNA-3B; Provisional


Pssm-ID: 223065 [Multi-domain]  Cd Length: 991  Bit Score: 52.76  E-value: 1.19e-06
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  955 KPTRKGMAKGRPRrsSQAPTRAAPTRAAPGPPRgmdrngvPPSARGGPLpleimsggsshRPPRG------PPSTSLGAS 1028
Cdd:PHA03378   675 QPSPTGANTMLPI--QWAPGTMQPPPRAPTPMR-------PPAAPPGRA-----------QRPAAatgrarPPAAAPGRA 734
                           90       100       110       120       130
                   ....*....|....*....|....*....|....*....|....*....|....*
gi 1622892340 1029 RRPRA---QLPSEHNTEFLNVPDQGMAGMQRKrsvgqrPVPGVGRPKPQPRTHGP 1080
Cdd:PHA03378   735 RPPAAapgRARPPAAAPGRARPPAAAPGRARP------PAAAPGAPTPQPPPQAP 783
SH3_CASS4 cd12000
Src homology 3 domain of CAS (Crk-Associated Substrate) scaffolding protein family member 4; ...
1083-1129 1.22e-06

Src homology 3 domain of CAS (Crk-Associated Substrate) scaffolding protein family member 4; CASS4, also called HEPL (HEF1-EFS-p130Cas-like), localizes to focal adhesions and plays a role in regulating FAK activity, focal adhesion integrity, and cell spreading. It is most abundant in blood cells and lung tissue, and is also found in high levels in leukemia and ovarian cell lines. CAS proteins function as molecular scaffolds to regulate protein complexes that are involved in many cellular processes. They share a common domain structure that includes an N-terminal SH3 domain, an unstructured substrate domain that contains many YxxP motifs, a serine-rich four-helix bundle, and a FAT-like C-terminal domain. The SH3 domain of CAS proteins binds to diverse partners including FAK, FRNK, Pyk2, PTP-PEST, DOCK180, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212933  Cd Length: 57  Bit Score: 46.41  E-value: 1.22e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMED---SSGWWKGRLHGQEGLFPGN 1129
Cdd:cd12000      4 RALYDNKADCSDELAFRRGDILTVLEQNvpgSEGWWKCLLHGRQGLAPAN 53
SH3_Nebulin_C cd11933
C-terminal Src Homology 3 domain of Nebulin; Nebulin is a giant filamentous protein (600-900 ...
1079-1134 1.39e-06

C-terminal Src Homology 3 domain of Nebulin; Nebulin is a giant filamentous protein (600-900 kD) that is expressed abundantly in skeletal muscle. It binds to actin thin filaments and regulates its assembly and function. Nebulin was thought to be part of a molecular ruler complex that is critical in determining the lengths of actin thin filaments in skeletal muscle since its length, which varies due to alternative splicing, correlates with the length of thin filaments in various muscle types. Recent studies indicate that nebulin regulates thin filament length by stabilizing the filaments and preventing depolymerization. Mutations in nebulin can cause nemaline myopathy, characterized by muscle weakness which can be severe and can lead to neonatal lethality. Nebulin contains an N-terminal LIM domain, many nebulin repeats/super repeats, and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212866 [Multi-domain]  Cd Length: 58  Bit Score: 46.54  E-value: 1.39e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*...
gi 1622892340 1079 GPRCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLH--GQEGLFPGNYVEKI 1134
Cdd:cd11933      1 GKSFRAMYDYRAADDDEVSFKDGDTIVNVQTIDEGWMYGTVQrtGKTGMLPANYVEAI 58
SH3_ephexin1_like cd11793
Src homology 3 domain of ephexin-1-like SH3 domain containing Rho guanine nucleotide exchange ...
1084-1132 1.59e-06

Src homology 3 domain of ephexin-1-like SH3 domain containing Rho guanine nucleotide exchange factors; Members of this family contain RhoGEF (also called Dbl-homologous or DH), Pleckstrin Homology (PH), and C-terminal SH3 domains. They include the Rho guanine nucleotide exchange factors ARHGEF5, ARHGEF16, ARHGEF19, ARHGEF26, ARHGEF27 (also called ephexin-1), and similar proteins, and are also called ephexins because they interact directly with ephrin A receptors. GEFs interact with Rho GTPases via their DH domains to catalyze nucleotide exchange by stabilizing the nucleotide-free GTPase intermediate. They play important roles in neuronal development. The SH3 domains of ARHGEFs play an autoinhibitory role through intramolecular interactions with a proline-rich region N-terminal to the DH domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212727 [Multi-domain]  Cd Length: 55  Bit Score: 46.17  E-value: 1.59e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKG-RLH-GQEGLFPGNYVE 1132
Cdd:cd11793      4 CVHAYTAQQPDELTLEEGDVVNVLRKMPDGWYEGeRLRdGERGWFPSSYTE 54
SH3_srGAP4 cd11956
Src homology 3 domain of Slit-Robo GTPase Activating Protein 4; srGAP4, also called ARHGAP4, ...
1084-1131 1.72e-06

Src homology 3 domain of Slit-Robo GTPase Activating Protein 4; srGAP4, also called ARHGAP4, is highly expressed in hematopoietic cells and may play a role in lymphocyte differentiation. It is able to stimulate the GTPase activity of Rac1, Cdc42, and RhoA. In the nervous system, srGAP4 has been detected in differentiating neurites and may be involved in axon and dendritic growth. srGAPs are Rho GAPs that interact with Robo1, the transmembrane receptor of Slit proteins. Slit proteins are secreted proteins that control axon guidance and the migration of neurons and leukocytes. srGAPs contain an N-terminal F-BAR domain, a Rho GAP domain, and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212889 [Multi-domain]  Cd Length: 55  Bit Score: 45.99  E-value: 1.72e-06
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*...
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11956      6 ACFDYTGRTAQELSFKRGDVLLLHSKASSDWWRGEHNGMRGLIPHKYI 53
SH3_SNX33 cd11896
Src Homology 3 domain of Sorting Nexin 33; SNX33 interacts with Wiskott-Aldrich syndrome ...
1081-1132 1.73e-06

Src Homology 3 domain of Sorting Nexin 33; SNX33 interacts with Wiskott-Aldrich syndrome protein (WASP) and plays a role in the maintenance of cell shape and cell cycle progression. It modulates the shedding and endocytosis of cellular prion protein (PrP(c)) and amyloid precursor protein (APP). SNXs are Phox homology (PX) domain containing proteins that are involved in regulating membrane traffic and protein sorting in the endosomal system. SNX33 also contains BAR and SH3 domains. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212829 [Multi-domain]  Cd Length: 55  Bit Score: 46.11  E-value: 1.73e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDS-SGWWKGR-LHGQEGLFPGNYVE 1132
Cdd:cd11896      1 KARALYSFQSENKEEINIQENEELVIFSENSlDGWLQGQnSRGETGLFPASYVE 54
SH3_Intersectin2_1 cd11988
First Src homology 3 domain (or SH3A) of Intersectin-2; Intersectin-2 (ITSN2) is an adaptor ...
1083-1133 2.00e-06

First Src homology 3 domain (or SH3A) of Intersectin-2; Intersectin-2 (ITSN2) is an adaptor protein that functions in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. It plays a role in clathrin-coated pit (CCP) formation. It binds to many proteins through its multidomain structure and facilitate the assembly of multimeric complexes. ITSN2 also functions as a specific GEF for Cdc42 activation in epithelial morphogenesis, and is required in mitotic spindle orientation. It exists in alternatively spliced short and long isoforms. The short isoform contains two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoform, in addition, contains RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. The first SH3 domain (or SH3A) of ITSN2 is expected to bind many protein partners, similar to ITSN1 which has been shown to bind Sos1, dynamin1/2, CIN85, c-Cbl, PI3K-C2, SHIP2, N-WASP, and CdGAP, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212921 [Multi-domain]  Cd Length: 57  Bit Score: 46.02  E-value: 2.00e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*.
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEIlmeDSS-----GWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11988      5 RALYPFEARNHDEMSFNAGDIIQV---DEKtvgepGWLYGSFQGNFGWFPCNYVEK 57
SH3_GRB2_N cd11946
N-terminal Src homology 3 domain of Growth factor receptor-bound protein 2; GRB2 is a critical ...
1084-1132 2.21e-06

N-terminal Src homology 3 domain of Growth factor receptor-bound protein 2; GRB2 is a critical signaling molecule that regulates the Ras pathway by linking tyrosine kinases to the Ras guanine nucleotide releasing protein Sos (son of sevenless), which converts Ras to the active GTP-bound state. It is ubiquitously expressed in all tissues throughout development and is important in cell cycle progression, motility, morphogenesis, and angiogenesis. In lymphocytes, GRB2 is associated with antigen receptor signaling components. GRB2 contains an N-terminal SH3 domain, a central SH2 domain, and a C-terminal SH3 domain. Its N-terminal SH3 domain binds to Sos and Sos-derived proline-rich peptides. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212879 [Multi-domain]  Cd Length: 56  Bit Score: 45.79  E-value: 2.21e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDS-SGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11946      5 AKYDFKATADDELSFKRGDILKVLNEECdQNWYKAELNGKDGFIPKNYIE 54
SH3_Nck2_2 cd11902
Second Src Homology 3 domain of Nck2 adaptor protein; Nck2 (also called Nckbeta or Growth ...
1086-1131 2.26e-06

Second Src Homology 3 domain of Nck2 adaptor protein; Nck2 (also called Nckbeta or Growth factor receptor-bound protein 4, Grb4) plays a crucial role in connecting signaling pathways of tyrosine kinase receptors and important effectors in actin dynamics and cytoskeletal remodeling. It binds neuronal signaling proteins such as ephrinB and Disabled-1 (Dab-1) exclusively. Nck adaptor proteins regulate actin cytoskeleton dynamics by linking proline-rich effector molecules to protein tyrosine kinases and phosphorylated signaling intermediates. They contain three SH3 domains and a C-terminal SH2 domain. They function downstream of the PDGFbeta receptor and are involved in Rho GTPase signaling and actin dynamics. Vertebrates contain two Nck adaptor proteins: Nck1 (also called Nckalpha) and Nck2, which show partly overlapping functions but also bind distinct targets. The second SH3 domain of Nck appears to prefer ligands containing the APxxPxR motif. SH3 domains are protein interaction domains that usually bind to proline-rich ligands with moderate affinity and selectivity, preferentially a PxxP motif. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212835 [Multi-domain]  Cd Length: 55  Bit Score: 45.77  E-value: 2.26e-06
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*.
gi 1622892340 1086 YQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11902      7 FAYVAEREDELSLVKGSRVTVMEKCSDGWWRGSYNGQIGWFPSNYV 52
PHA03378 PHA03378
EBNA-3B; Provisional
962-1080 2.29e-06

EBNA-3B; Provisional


Pssm-ID: 223065 [Multi-domain]  Cd Length: 991  Bit Score: 51.99  E-value: 2.29e-06
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  962 AKGRPRRSSQAPTRAAPTRAAPGPPRgmdrngvPPSARGGPLPLEIMSGGSSHRP-----PRGPPSTSLGASRRPRA--- 1033
Cdd:PHA03378   690 APGTMQPPPRAPTPMRPPAAPPGRAQ-------RPAAATGRARPPAAAPGRARPPaaapgRARPPAAAPGRARPPAAapg 762
                           90       100       110       120       130
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1034 QLPSEHNTEFLNVPDQ----GMAGMQRKRsvgqrpvpgvGRPKPQPRTHGP 1080
Cdd:PHA03378   763 RARPPAAAPGAPTPQPppqaPPAPQQRPR----------GAPTPQPPPQAG 803
SH3_EFS cd12003
Src homology 3 domain of CAS (Crk-Associated Substrate) scaffolding protein family member, ...
1083-1134 2.34e-06

Src homology 3 domain of CAS (Crk-Associated Substrate) scaffolding protein family member, Embryonal Fyn-associated Substrate; EFS is also called HEFS, CASS3 (Cas scaffolding protein family member 3) or SIN (Src-interacting protein). It was identified based on interactions with the Src kinases, Fyn and Yes. It plays a role in thymocyte development and acts as a negative regulator of T cell proliferation. CAS proteins function as molecular scaffolds to regulate protein complexes that are involved in many cellular processes. They share a common domain structure that includes an N-terminal SH3 domain, an unstructured substrate domain that contains many YxxP motifs, a serine-rich four-helix bundle, and a FAT-like C-terminal domain. The SH3 domain of CAS proteins binds to diverse partners including FAK, FRNK, Pyk2, PTP-PEST, DOCK180, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212936  Cd Length: 62  Bit Score: 46.04  E-value: 2.34e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSS---GWWKGRLHGQEGLFPGNYVEKI 1134
Cdd:cd12003      4 KALYDNAAESPEELSFRRGDVLMVLKREHGslpGWWLCSLHGQQGIAPANRLRLL 58
SH3_Stac_1 cd11833
First C-terminal Src homology 3 domain of SH3 and cysteine-rich domain-containing (Stac) ...
1084-1133 2.41e-06

First C-terminal Src homology 3 domain of SH3 and cysteine-rich domain-containing (Stac) proteins; Stac proteins are putative adaptor proteins that contain a cysteine-rich C1 domain and one or two SH3 domains at the C-terminus. There are three mammalian members (Stac1, Stac2, and Stac3) of this family. Stac1 and Stac3 contain two SH3 domains while Stac2 contains a single SH3 domain at the C-terminus. This model represents the first C-terminal SH3 domain of Stac1 and Stac3, and the single C-terminal SH3 domain of Stac2. Stac1 and Stac2 have been found to be expressed differently in mature dorsal root ganglia (DRG) neurons. Stac1 is mainly expressed in peptidergic neurons while Stac2 is found in a subset of nonpeptidergic and all trkB+ neurons. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212767 [Multi-domain]  Cd Length: 53  Bit Score: 45.57  E-value: 2.41e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11833      4 ALYKFKPQENEDLEMRPGDKITLLDDSNEDWWKGKIEDRVGFFPANFVQR 53
SH3_Stac2_C cd11985
C-terminal Src homology 3 domain of SH3 and cysteine-rich domain-containing protein 2 (Stac2); ...
1084-1133 2.64e-06

C-terminal Src homology 3 domain of SH3 and cysteine-rich domain-containing protein 2 (Stac2); Stac proteins are putative adaptor proteins that contain a cysteine-rich C1 domain and one or two SH3 domains at the C-terminus. There are three mammalian members (Stac1, Stac2, and Stac3) of this family. Stac2 contains a single SH3 domain at the C-terminus unlike Stac1 and Stac3, which contain two C-terminal SH3 domains. Stac1 and Stac2 have been found to be expressed differently in mature dorsal root ganglia (DRG) neurons. Stac1 is mainly expressed in peptidergic neurons while Stac2 is found in a subset of nonpeptidergic and all trkB+ neurons. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212918  Cd Length: 53  Bit Score: 45.71  E-value: 2.64e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11985      4 ALYKFLPQENNDLPLQPGDRVMVVDDSNEDWWKGKSGDRVGFFPANFVQR 53
SH3_Intersectin2_3 cd11992
Third Src homology 3 domain (or SH3C) of Intersectin-2; Intersectin-2 (ITSN2) is an adaptor ...
1084-1131 2.91e-06

Third Src homology 3 domain (or SH3C) of Intersectin-2; Intersectin-2 (ITSN2) is an adaptor protein that functions in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. It plays a role in clathrin-coated pit (CCP) formation. It binds to many proteins through its multidomain structure and facilitate the assembly of multimeric complexes. ITSN2 also functions as a specific GEF for Cdc42 activation in epithelial morphogenesis, and is required in mitotic spindle orientation. It exists in alternatively spliced short and long isoforms. The short isoform contains two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoform, in addition, contains RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. The third SH3 domain (SH3C) of ITSN2 has been shown to bind the K15 protein of Kaposi's sarcoma-associated herpesvirus. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212925  Cd Length: 52  Bit Score: 45.39  E-value: 2.91e-06
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*...
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSgWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11992      4 ALYPYSSSEPGDLTFNEGEEILVTQKDGE-WWTGSIEDRTGIFPSNYV 50
SH3_Intersectin1_2 cd11989
Second Src homology 3 domain (or SH3B) of Intersectin-1; Intersectin-1 (ITSN1) is an adaptor ...
1081-1132 3.04e-06

Second Src homology 3 domain (or SH3B) of Intersectin-1; Intersectin-1 (ITSN1) is an adaptor protein that functions in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. It plays a role in clathrin-coated pit (CCP) formation. It binds to many proteins through its multidomain structure and facilitate the assembly of multimeric complexes. ITSN1 localizes in membranous organelles, CCPs, the Golgi complex, and may be involved in the cell membrane trafficking system. It exists in alternatively spliced short and long isoforms. The short isoform contains two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoform, in addition, contains RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. The second SH3 domain (or SH3B) of ITSN1 has been shown to bind WNK and CdGAP. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212922 [Multi-domain]  Cd Length: 52  Bit Score: 45.48  E-value: 3.04e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|..
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILmEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11989      1 QAQALYPWRAKKDNHLNFNKNDVITVL-EQQDMWWFGEVQGQKGWFPKSYVK 51
PHA03378 PHA03378
EBNA-3B; Provisional
951-1085 3.06e-06

EBNA-3B; Provisional


Pssm-ID: 223065 [Multi-domain]  Cd Length: 991  Bit Score: 51.61  E-value: 3.06e-06
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  951 PKSSKPTRK---GMAKGRPRRSSQAPTRAAPTRAAPG---PPRGMDRNGVPPSARGGPLPLEIMSGGSS--HRPPRGPPS 1022
Cdd:PHA03378   706 PPAAPPGRAqrpAAATGRARPPAAAPGRARPPAAAPGrarPPAAAPGRARPPAAAPGRARPPAAAPGAPtpQPPPQAPPA 785
                           90       100       110       120       130       140       150
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|..
gi 1622892340 1023 tslgASRRPRA-----QLPSEHNTEFLNVPDQgMAGMQ--RKRSVGQRPVPGV--GRPKPQPRTHGPRCRAL 1085
Cdd:PHA03378   786 ----PQQRPRGaptpqPPPQAGPTSMQLMPRA-APGQQgpTKQILRQLLTGGVkrGRPSLKKPAALERQAAA 852
SH3_Lyn cd12004
Src homology 3 domain of Lyn Protein Tyrosine Kinase; Lyn is a member of the Src subfamily of ...
1084-1134 3.35e-06

Src homology 3 domain of Lyn Protein Tyrosine Kinase; Lyn is a member of the Src subfamily of proteins, which are cytoplasmic (or non-receptor) PTKs. Lyn is expressed in B lymphocytes and myeloid cells. It exhibits both positive and negative regulatory roles in B cell receptor (BCR) signaling. Lyn, as well as Fyn and Blk, promotes B cell activation by phosphorylating ITAMs (immunoreceptor tyr activation motifs) in CD19 and in Ig components of BCR. It negatively regulates signaling by its unique ability to phosphorylate ITIMs (immunoreceptor tyr inhibition motifs) in cell surface receptors like CD22 and CD5. Lyn also plays an important role in G-CSF receptor signaling by phosphorylating a variety of adaptor molecules. Src kinases contain an N-terminal SH4 domain with a myristoylation site, followed by SH3 and SH2 domains, a tyr kinase domain, and a regulatory C-terminal region containing a conserved tyr. They are activated by autophosphorylation at the tyr kinase domain, but are negatively regulated by phosphorylation at the C-terminal tyr by Csk (C-terminal Src Kinase). The SH3 domain of Src kinases contributes to substrate recruitment by binding adaptor proteins/substrates, and regulation of kinase activity through an intramolecular interaction. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212937 [Multi-domain]  Cd Length: 56  Bit Score: 45.37  E-value: 3.35e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|...
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILmEDSSGWWKGR--LHGQEGLFPGNYVEKI 1134
Cdd:cd12004      4 ALYPYDGIHEDDLSFKKGEKLKVI-EEHGEWWKARslTTKKEGFIPSNYVAKV 55
SH3_Sorbs1_3 cd11916
Third (or C-terminal) Src Homology 3 domain of Sorbin and SH3 domain containing 1 (Sorbs1), ...
1083-1132 3.56e-06

Third (or C-terminal) Src Homology 3 domain of Sorbin and SH3 domain containing 1 (Sorbs1), also called ponsin; Sorbs1 is also called ponsin, SH3P12, or CAP (c-Cbl associated protein). It is an adaptor protein containing one sorbin homology (SoHo) and three SH3 domains. It binds Cbl and plays a major role in regulating the insulin signaling pathway by enhancing insulin-induced phosphorylation of Cbl. Sorbs1, like vinexin, localizes at cell-ECM and cell-cell adhesion sites where it binds vinculin, paxillin, and afadin. It may function in the control of cell motility. Other interaction partners of Sorbs1 include c-Abl, Sos, flotillin, Grb4, ataxin-7, filamin C, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212849 [Multi-domain]  Cd Length: 59  Bit Score: 45.37  E-value: 3.56e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|..
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKG--RLHGQEGLFPGNYVE 1132
Cdd:cd11916      5 QALYSYAPQNDDELELRDGDIVDVMEKCDDGWFVGtsRRTKQFGTFPGNYVK 56
SH3_Tks_2 cd12016
Second Src homology 3 domain of Tyrosine kinase substrate (Tks) proteins; Tks proteins are Src ...
1086-1133 3.59e-06

Second Src homology 3 domain of Tyrosine kinase substrate (Tks) proteins; Tks proteins are Src substrates and scaffolding proteins that play important roles in the formation of podosomes and invadopodia, the dynamic actin-rich structures that are related to cell migration and cancer cell invasion. Vertebrates contain two Tks proteins, Tks4 (Tyr kinase substrate with four SH3 domains) and Tks5 (Tyr kinase substrate with five SH3 domains), which display partially overlapping but non-redundant functions. Both associate with the ADAMs family of transmembrane metalloproteases, which function as sheddases and mediators of cell and matrix interactions. Tks5 interacts with N-WASP and Nck, while Tks4 is essential for the localization of MT1-MMP (membrane-type 1 matrix metalloproteinase) to invadopodia. Tks proteins contain an N-terminal Phox homology (PX) domain and four or five SH3 domains. This model characterizes the second SH3 domain of Tks proteins. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212949  Cd Length: 54  Bit Score: 45.14  E-value: 3.59e-06
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*...
gi 1622892340 1086 YQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd12016      7 QAYKAENEDEIGFETGVVVEVIQKNLDGWWKIRYQGKEGWAPATYLKK 54
PHA03247 PHA03247
large tegument protein UL36; Provisional
940-1079 3.80e-06

large tegument protein UL36; Provisional


Pssm-ID: 223021 [Multi-domain]  Cd Length: 3151  Bit Score: 51.48  E-value: 3.80e-06
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  940 RTLTVSVGDGLPKSSKPTRKGMAKGRPRRSSQAPTRAAPTRAAPGPPRGMDRNGVP--PSARGGPLPLEIMSGGS----- 1012
Cdd:PHA03247  2781 RRLTRPAVASLSESRESLPSPWDPADPPAAVLAPAAALPPAASPAGPLPPPTSAQPtaPPPPPGPPPPSLPLGGSvapgg 2860
                           90       100       110       120       130       140       150
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1622892340 1013 --SHRPPRGPPSTSLGASRRPR----AQLPSEHNTEFLNVPDQGMAGMQR----KRSVGQRPVPGVGRPKPQPRTHG 1079
Cdd:PHA03247  2861 dvRRRPPSRSPAAKPAAPARPPvrrlARPAVSRSTESFALPPDQPERPPQpqapPPPQPQPQPPPPPQPQPPPPPPP 2937
SH3_Nck1_2 cd11901
Second Src Homology 3 domain of Nck1 adaptor protein; Nck1 (also called Nckalpha) plays a ...
1086-1131 4.70e-06

Second Src Homology 3 domain of Nck1 adaptor protein; Nck1 (also called Nckalpha) plays a crucial role in connecting signaling pathways of tyrosine kinase receptors and important effectors in actin dynamics and cytoskeletal remodeling. It binds and activates RasGAP, resulting in the downregulation of Ras. It is also involved in the signaling of endothilin-mediated inhibition of cell migration. Nck adaptor proteins regulate actin cytoskeleton dynamics by linking proline-rich effector molecules to protein tyrosine kinases and phosphorylated signaling intermediates. They contain three SH3 domains and a C-terminal SH2 domain. They function downstream of the PDGFbeta receptor and are involved in Rho GTPase signaling and actin dynamics. Vertebrates contain two Nck adaptor proteins: Nck1 (also called Nckalpha) and Nck2, which show partly overlapping functions but also bind distinct targets. The second SH3 domain of Nck appears to prefer ligands containing the APxxPxR motif. SH3 domains are protein interaction domains that usually bind to proline-rich ligands with moderate affinity and selectivity, preferentially a PxxP motif. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212834 [Multi-domain]  Cd Length: 55  Bit Score: 45.03  E-value: 4.70e-06
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*..
gi 1622892340 1086 YQYVGQDVDELSFnVNEVIEILMED-SSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11901      8 FNYTAEREDELSL-VKGTKVIVMEKcSDGWWRGSYNGQVGWFPSNYV 53
SH3_Sla1p_2 cd11774
Second Src Homology 3 domain of the fungal endocytic adaptor protein Sla1p; Sla1p facilitates ...
1083-1131 5.03e-06

Second Src Homology 3 domain of the fungal endocytic adaptor protein Sla1p; Sla1p facilitates endocytosis by playing a role as an adaptor protein in coupling components of the actin cytoskeleton to the endocytic machinery. It interacts with Abp1p, Las17p and Pan1p, which are activator proteins of actin-related protein 2/3 (Arp2/3). Sla1p contains multiple domains including three SH3 domains, a SAM (sterile alpha motif) domain, and a Sla1 homology domain 1 (SHD1), which binds to the NPFXD motif that is found in many integral membrane proteins such as the Golgi-localized Arf-binding protein Lsb5p and the P4-ATPases, Drs2p and Dnf1p. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212708 [Multi-domain]  Cd Length: 52  Bit Score: 44.76  E-value: 5.03e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQE-GLFPGNYV 1131
Cdd:cd11774      3 KALYDYDKQTEEELSFNEGDTLDVYDDSDSDWILVGFNGTQfGFVPANYI 52
SH3_BTK cd11906
Src Homology 3 domain of Bruton's tyrosine kinase; BTK is a cytoplasmic (or nonreceptor) tyr ...
1084-1131 6.18e-06

Src Homology 3 domain of Bruton's tyrosine kinase; BTK is a cytoplasmic (or nonreceptor) tyr kinase containing Src homology protein interaction domains (SH3, SH2) N-terminal to the catalytic tyr kinase domain. It also contains an N-terminal pleckstrin homology (PH) domain, which binds the products of PI3K and allows membrane recruitment and activation, and the Tec homology (TH) domain with proline-rich and zinc-binding regions. Btk is expressed in B-cells, and a variety of myeloid cells including mast cells, platelets, neutrophils, and dendrictic cells. It interacts with a variety of partners, from cytosolic proteins to nuclear transcription factors, suggesting a diversity of functions. Stimulation of a diverse array of cell surface receptors, including antigen engagement of the B-cell receptor (BCR), leads to PH-mediated membrane translocation of Btk and subsequent phosphorylation by Src kinase and activation. Btk plays an important role in the life cycle of B-cells including their development, differentiation, proliferation, survival, and apoptosis. Mutations in Btk cause the primary immunodeficiency disease, X-linked agammaglobulinaemia (XLA) in humans. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212839 [Multi-domain]  Cd Length: 55  Bit Score: 44.43  E-value: 6.18e-06
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGR-LHGQEGLFPGNYV 1131
Cdd:cd11906      5 ALYDYTPMNAQDLQLRKGEEYVILEESNLPWWRARdKNGREGYIPSNYV 53
SH3_Src_like cd11845
Src homology 3 domain of Src kinase-like Protein Tyrosine Kinases; Src subfamily members ...
1083-1130 6.74e-06

Src homology 3 domain of Src kinase-like Protein Tyrosine Kinases; Src subfamily members include Src, Lck, Hck, Blk, Lyn, Fgr, Fyn, Yrk, Yes, and Brk. Src (or c-Src) proteins are cytoplasmic (or non-receptor) PTKs which are anchored to the plasma membrane. They contain an N-terminal SH4 domain with a myristoylation site, followed by SH3 and SH2 domains, a tyr kinase domain, and a regulatory C-terminal region containing a conserved tyr. They are activated by autophosphorylation at the tyr kinase domain, but are negatively regulated by phosphorylation at the C-terminal tyr by Csk (C-terminal Src Kinase). However, Brk lacks the N-terminal myristoylation sites. Src proteins are involved in signaling pathways that regulate cytokine and growth factor responses, cytoskeleton dynamics, cell proliferation, survival, and differentiation. They were identified as the first proto-oncogene products, and they regulate cell adhesion, invasion, and motility in cancer cells, and tumor vasculature, contributing to cancer progression and metastasis. Src kinases are overexpressed in a variety of human cancers, making them attractive targets for therapy. They are also implicated in acute inflammatory responses and osteoclast function. Src, Fyn, Yes, and Yrk are widely expressed, while Blk, Lck, Hck, Fgr, Lyn, and Brk show a limited expression pattern. This subfamily also includes Drosophila Src42A, Src oncogene at 42A (also known as Dsrc41) which accumulates at sites of cell-cell or cell-matrix adhesion, and participates in Drosphila development and wound healing. It has been shown to promote tube elongation in the tracheal system, is essential for proper cell-cell matching during dorsal closure, and regulates cell-cell contacts in developing Drosophila eyes. The SH3 domain of Src kinases contributes to substrate recruitment by binding adaptor proteins/substrates, and regulation of kinase activity through an intramolecular interaction. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212779 [Multi-domain]  Cd Length: 52  Bit Score: 44.11  E-value: 6.74e-06
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRL--HGQEGLFPGNY 1130
Cdd:cd11845      3 VALYDYEARTDDDLSFKKGDRLQILDDSDGDWWLARHlsTGKEGYIPSNY 52
SH3_SNX18 cd11897
Src Homology 3 domain of Sorting nexin 18; SNX18 is localized to peripheral endosomal ...
1081-1132 7.11e-06

Src Homology 3 domain of Sorting nexin 18; SNX18 is localized to peripheral endosomal structures, and acts in a trafficking pathway that is clathrin-independent but relies on AP-1 and PACS1. It binds FIP5 and is required for apical lumen formation. It may also play a role in axonal elongation. SNXs are Phox homology (PX) domain containing proteins that are involved in regulating membrane traffic and protein sorting in the endosomal system. SNX18 also contains BAR and SH3 domains. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212830 [Multi-domain]  Cd Length: 55  Bit Score: 44.21  E-value: 7.11e-06
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILME-DSSGWWKG-RLHGQEGLFPGNYVE 1132
Cdd:cd11897      1 RARALYDFRSENPGEISLREHEVLSLCSEqDIEGWLEGvNSRGDRGLFPASYVE 54
PHA03307 PHA03307
transcriptional regulator ICP4; Provisional
938-1083 8.29e-06

transcriptional regulator ICP4; Provisional


Pssm-ID: 223039 [Multi-domain]  Cd Length: 1352  Bit Score: 50.17  E-value: 8.29e-06
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gi 1622892340  938 GGRTLTVSVGDGLPKSSKPTRKGMAKGRPRRSSQAPTRAAPTRAAPGPPrgmdrngvPPSARGGPLPleiMSGGSSHRPP 1017
Cdd:PHA03307    81 ANESRSTPTWSLSTLAPASPAREGSPTPPGPSSPDPPPPTPPPASPPPS--------PAPDLSEMLR---PVGSPGPPPA 149
                           90       100       110       120       130       140
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gi 1622892340 1018 RGPPSTSLGASRRPRAQLPSEHNTEFLNVPDQGmagmqrKRSVGQRPVPGVGRPKPQPRTHGPRCR 1083
Cdd:PHA03307   150 ASPPAAGASPAAVASDAASSRQAALPLSSPEET------ARAPSSPPAEPPPSTPPAAASPRPPRR 209
SH3_Sla1p_3 cd11775
Third Src Homology 3 domain of the fungal endocytic adaptor protein Sla1p; Sla1p facilitates ...
1081-1132 8.74e-06

Third Src Homology 3 domain of the fungal endocytic adaptor protein Sla1p; Sla1p facilitates endocytosis by playing a role as an adaptor protein in coupling components of the actin cytoskeleton to the endocytic machinery. It interacts with Abp1p, Las17p and Pan1p, which are activator proteins of actin-related protein 2/3 (Arp2/3). Sla1p contains multiple domains including three SH3 domains, a SAM (sterile alpha motif) domain, and a Sla1 homology domain 1 (SHD1), which binds to the NPFXD motif that is found in many integral membrane proteins such as the Golgi-localized Arf-binding protein Lsb5p and the P4-ATPases, Drs2p and Dnf1p. The third SH3 domain of Sla1p can bind ubiquitin while retaining the ability to bind proline-rich ligands; monoubiquitination of target proteins signals internalization and sorting through the endocytic pathway. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212709 [Multi-domain]  Cd Length: 57  Bit Score: 44.23  E-value: 8.74e-06
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEIL-MEDSSGWWKGRL--HGQEGLFPGNYVE 1132
Cdd:cd11775      2 RGKVLYDFDAQSDDELTVKEGDVVYILdDKKSKDWWMVENvsTGKEGVVPASYIE 56
SH3_DNMBP_C2 cd12141
Second C-terminal Src homology 3 domain of Dynamin Binding Protein, also called Tuba, and ...
1084-1133 9.57e-06

Second C-terminal Src homology 3 domain of Dynamin Binding Protein, also called Tuba, and similar domains; DNMBP or Tuba is a cdc42-specific guanine nucleotide exchange factor (GEF) that contains four N-terminal SH3 domains, a central RhoGEF [or Dbl homology (DH)] domain followed by a Bin/Amphiphysin/Rvs (BAR) domain, and two C-terminal SH3 domains. It provides a functional link between dynamin, Rho GTPase signaling, and actin dynamics. It plays an important role in regulating cell junction configuration. The C-terminal SH3 domains of DNMBP bind to N-WASP and Ena/VASP proteins, which are key regulatory proteins of the actin cytoskeleton. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 213017 [Multi-domain]  Cd Length: 57  Bit Score: 44.03  E-value: 9.57e-06
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEIL-MEDSSG---WWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd12141      4 AVYTFKARSPNELSVSANQRVRILeFSDLTGnkeWWLAEANGQKGYVPSNYIRK 57
SH3_Tks5_2 cd12077
Second Src homology 3 domain of Tyrosine kinase substrate with five SH3 domains; Tks5, also ...
1088-1133 1.07e-05

Second Src homology 3 domain of Tyrosine kinase substrate with five SH3 domains; Tks5, also called SH3 and PX domain-containing protein 2A (SH3PXD2A) or Five SH (FISH), is a scaffolding protein and Src substrate that is localized in podosomes, which are electron-dense structures found in Src-transformed fibroblasts, osteoclasts, macrophages, and some invasive cancer cells. It binds and regulates some members of the ADAMs family of transmembrane metalloproteases, which function as sheddases and mediators of cell and matrix interactions. It is required for podosome formation, degradation of the extracellular matrix, and cancer cell invasion. Tks5 contains an N-terminal Phox homology (PX) domain and five SH3 domains. This model characterizes the second SH3 domain of Tks5. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 213010  Cd Length: 54  Bit Score: 43.87  E-value: 1.07e-05
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gi 1622892340 1088 YVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd12077      9 YTSQGKDEIGFEKGVTVEVIQKNLEGWWYIRYLGKEGWAPASYLKK 54
SH3_SH3RF1_1 cd11927
First Src Homology 3 domain of SH3 domain containing ring finger protein 1, an E3 ...
1080-1132 1.16e-05

First Src Homology 3 domain of SH3 domain containing ring finger protein 1, an E3 ubiquitin-protein ligase; SH3RF1 is also called POSH (Plenty of SH3s) or SH3MD2 (SH3 multiple domains protein 2). It is a scaffold protein that acts as an E3 ubiquitin-protein ligase. It plays a role in calcium homeostasis through the control of the ubiquitin domain protein Herp. It may also have a role in regulating death receptor mediated and JNK mediated apoptosis. SH3RF1 also enhances the ubiquitination of ROMK1 potassium channel resulting in its increased endocytosis. It contains an N-terminal RING finger domain and four SH3 domains. This model represents the first SH3 domain, located at the N-terminal half, of SH3RF1. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212860  Cd Length: 54  Bit Score: 43.79  E-value: 1.16e-05
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gi 1622892340 1080 PRCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11927      1 PCAKALYNYEGKEPGDLKFSKGDIIILRRQVDENWYHGEVNGIHGFFPTNFVQ 53
SH3_ASEF cd11973
Src homology 3 domain of APC-Stimulated guanine nucleotide Exchange Factor; ASEF, also called ...
1084-1131 1.29e-05

Src homology 3 domain of APC-Stimulated guanine nucleotide Exchange Factor; ASEF, also called ARHGEF4, exists in an autoinhibited form and is activated upon binding of the tumor suppressor APC (adenomatous polyposis coli). GEFs activate small GTPases by exchanging bound GDP for free GTP. ASEF can activate Rac1 or Cdc42. Truncated ASEF, which is found in colorectal cancers, is constitutively active and has been shown to promote angiogenesis and cancer cell migration. ASEF contains a SH3 domain followed by RhoGEF (also called Dbl-homologous or DH) and Pleckstrin Homology (PH) domains. In its autoinhibited form, the SH3 domain of ASEF forms an extensive interface with the DH and PH domains, blocking the Rac binding site. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212906 [Multi-domain]  Cd Length: 73  Bit Score: 44.24  E-value: 1.29e-05
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11973     22 ALWDHVTMDDQELGFKAGDVIEVMDATNKEWWWGRVLDSEGWFPASFV 69
SH3_Eve1_2 cd11815
Second Src homology 3 domain of ADAM-binding protein Eve-1; Eve-1, also called SH3 ...
1085-1132 1.30e-05

Second Src homology 3 domain of ADAM-binding protein Eve-1; Eve-1, also called SH3 domain-containing protein 19 (SH3D19) or EEN-binding protein (EBP), exists in multiple alternatively spliced isoforms. The longest isoform contains five SH3 domain in the C-terminal region and seven proline-rich motifs in the N-terminal region. It is abundantly expressed in skeletal muscle and heart, and may be involved in regulating the activity of ADAMs (A disintegrin and metalloproteases). Eve-1 interacts with EEN, an endophilin involved in endocytosis and may be the target of the MLL-EEN fusion protein that is implicated in leukemogenesis. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212749 [Multi-domain]  Cd Length: 52  Bit Score: 43.71  E-value: 1.30e-05
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gi 1622892340 1085 LYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11815      5 LHDFPAEHSDDLSLNSGEIVYLLEKIDTEWYRGKCKNTTGIFPANHVK 52
SH3_FNBP1L cd12072
Src Homology 3 domain of Formin Binding Protein 1-Like; FormiN Binding Protein 1-Like (FNBP1L), ...
1082-1132 1.53e-05

Src Homology 3 domain of Formin Binding Protein 1-Like; FormiN Binding Protein 1-Like (FNBP1L), also known as Toca-1 (Transducer of Cdc42-dependent actin assembly), forms a complex with neural Wiskott-Aldrich syndrome protein (N-WASP). The FNBP1L/N-WASP complex induces the formation of filopodia and endocytic vesicles. FNBP1L is required for Cdc42-induced actin assembly and is essential for autophagy of intracellular pathogens. It contains an N-terminal F-BAR domain, a central Cdc42-binding HR1 domain, and a C-terminal SH3 domain. The SH3 domain of the related protein, CIP4, associates with Gapex-5, a Rab31 GEF. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 213005 [Multi-domain]  Cd Length: 57  Bit Score: 43.44  E-value: 1.53e-05
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gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMEDS-SGWWKGRLH-GQEGLFPGNYVE 1132
Cdd:cd12072      3 CKALYPFDGSNEGTLAMKEGEVLYIIEEDKgDGWTRARKQnGEEGYVPTSYIE 55
SH3_Nck1_3 cd11904
Third Src Homology 3 domain of Nck1 adaptor protein; Nck1 (also called Nckalpha) plays a ...
1083-1131 1.78e-05

Third Src Homology 3 domain of Nck1 adaptor protein; Nck1 (also called Nckalpha) plays a crucial role in connecting signaling pathways of tyrosine kinase receptors and important effectors in actin dynamics and cytoskeletal remodeling. It binds and activates RasGAP, resulting in the downregulation of Ras. It is also involved in the signaling of endothilin-mediated inhibition of cell migration. Nck adaptor proteins regulate actin cytoskeleton dynamics by linking proline-rich effector molecules to protein tyrosine kinases and phosphorylated signaling intermediates. They contain three SH3 domains and a C-terminal SH2 domain. They function downstream of the PDGFbeta receptor and are involved in Rho GTPase signaling and actin dynamics. Vertebrates contain two Nck adaptor proteins: Nck1 (also called Nckalpha) and Nck2, which show partly overlapping functions but also bind distinct targets. The third SH3 domain of Nck appears to prefer ligands with a PxAPxR motif. SH3 domains are protein interaction domains that usually bind to proline-rich ligands with moderate affinity and selectivity, preferentially a PxxP motif. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212837 [Multi-domain]  Cd Length: 57  Bit Score: 43.48  E-value: 1.78e-05
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILM--EDSSGWWKGR-LHGQEGLFPGNYV 1131
Cdd:cd11904      4 QALYPFSSSNDEELNFEKGEVMDVIEkpENDPEWWKCRkANGQVGLVPKNYV 55
SH3_Vinexin_3 cd11918
Third (or C-terminal) Src Homology 3 domain of Vinexin, also called Sorbin and SH3 domain ...
1083-1134 1.81e-05

Third (or C-terminal) Src Homology 3 domain of Vinexin, also called Sorbin and SH3 domain containing 3 (Sorbs3); Vinexin is also called Sorbs3, SH3P3, and SH3-containing adapter molecule 1 (SCAM-1). It is an adaptor protein containing one sorbin homology (SoHo) and three SH3 domains. Vinexin was first identified as a vinculin binding protein; it is co-localized with vinculin at cell-ECM and cell-cell adhesion sites. There are several splice variants of vinexin: alpha, which contains the SoHo and three SH3 domains and displays tissue-specific expression; and beta, which contains only the three SH3 domains and is widely expressed. Vinexin alpha stimulates the accumulation of F-actin at focal contact sites. Vinexin also promotes keratinocyte migration and wound healing. The SH3 domains of vinexin have been reported to bind a number of ligands including vinculin, WAVE2, DLG5, Abl, and Cbl. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212851 [Multi-domain]  Cd Length: 58  Bit Score: 43.41  E-value: 1.81e-05
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKG--RLHGQEGLFPGNYVEKI 1134
Cdd:cd11918      5 KAVYQYRPQNEDELELREGDRVDVMQQCDDGWFVGvsRRTQKFGTFPGNYVAPV 58
SH3_ASPP1 cd11954
Src Homology 3 domain of Apoptosis Stimulating of p53 protein 1; ASPP1, like ASPP2, activates ...
1084-1129 1.86e-05

Src Homology 3 domain of Apoptosis Stimulating of p53 protein 1; ASPP1, like ASPP2, activates the apoptotic function of the p53 family of tumor suppressors (p53, p63, and p73). In addition, it functions in the cytoplasm to regulate the nuclear localization of the transcriptional cofactors YAP and TAZ by inihibiting their phosphorylation; YAP and TAZ are important regulators of cell expansion, differentiation, migration, and invasion. ASPP1 is downregulated in breast tumors expressing wild-type p53. It contains a proline-rich region, four ankyrin (ANK) repeats, and an SH3 domain at its C-terminal half. The SH3 domain and the ANK repeats of ASPP1 contribute to the p53 binding site; they bind to the DNA binding domain of p53. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212887 [Multi-domain]  Cd Length: 57  Bit Score: 43.08  E-value: 1.86e-05
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILM---EDSSGWWKGRLHGQEGLFPGN 1129
Cdd:cd11954      5 ALWDYEAQNADELSFQEGDAITILRrkdDSETEWWWARLNDKEGYVPKN 53
SH3_ephexin1 cd11939
Src homology 3 domain of the Rho guanine nucleotide exchange factor, ephexin-1 (also called ...
1085-1133 2.12e-05

Src homology 3 domain of the Rho guanine nucleotide exchange factor, ephexin-1 (also called NGEF or ARHGEF27); Ephexin-1, also called NGEF (neuronal GEF) or ARHGEF27, activates RhoA, Tac1, and Cdc42 by exchanging bound GDP for free GTP. It is expressed mainly in the brain in a region associated with movement control. It regulates the stability of postsynaptic acetylcholine receptor (AChR) clusters and thus, plays a critical role in the maturation and neurotransmission of neuromuscular junctions. Ephexin-1 directly interacts with the ephrin receptor EphA4 and their coexpression enhances the ability of ephexin-1 to activate RhoA. It is required for normal axon growth and EphA-induced growth cone collapse. Ephexin-1 contains RhoGEF (also called Dbl-homologous or DH), Pleckstrin Homology (PH), and SH3 domains. The SH3 domains of ARHGEFs play an autoinhibitory role through intramolecular interactions with a proline-rich region N-terminal to the DH domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212872 [Multi-domain]  Cd Length: 55  Bit Score: 43.01  E-value: 2.12e-05
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gi 1622892340 1085 LYQYVGQDVDELSFNVNEVIEILMEDSSGWWKG-RLHGQE-GLFPGNYVEK 1133
Cdd:cd11939      5 VHPYVSQEPDELSLELADVLNILDKTDDGWIFGeRLHDQErGWFPSSVVEE 55
SH3_GRAF2 cd12065
Src Homology 3 domain of GTPase Regulator Associated with Focal adhesion kinase 2; GRAF2, also ...
1081-1132 2.15e-05

Src Homology 3 domain of GTPase Regulator Associated with Focal adhesion kinase 2; GRAF2, also called Rho GTPase activating protein 10 (ARHGAP10) or PS-GAP, is a GAP with activity towards Cdc42 and RhoA. It regulates caspase-activated p21-activated protein kinase-2 (PAK-2p34). GRAF2 interacts with PAK-2p34, leading to its stabilization and decrease of cell death. It is highly expressed in skeletal muscle, and is involved in alpha-catenin recruitment at cell-cell junctions. GRAF2 contains an N-terminal BAR domain, followed by a Pleckstrin homology (PH) domain, a Rho GAP domain, and a C-terminal SH3 domain. The SH3 domain of GRAF binds PKNbeta, a target of the small GTPase Rho. SH3 domains bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs; they play a role in the regulation of enzymes by intramolecular interactions, changing the subcellular localization of signal pathway components and mediate multiprotein complex assemblies.


Pssm-ID: 212998 [Multi-domain]  Cd Length: 54  Bit Score: 43.05  E-value: 2.15e-05
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIE-ILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd12065      1 KAKAVYPCEAEHSSELSFEVGAIFEdVTLSREPGWLEGTLNGKRGLIPENYVE 53
SH3_srGAP1-3 cd11955
Src homology 3 domain of Slit-Robo GTPase Activating Proteins 1, 2, and 3; srGAP1, also called ...
1084-1131 2.36e-05

Src homology 3 domain of Slit-Robo GTPase Activating Proteins 1, 2, and 3; srGAP1, also called Rho GTPase-Activating Protein 13 (ARHGAP13), is a Cdc42- and RhoA-specific GAP and is expressed later in the development of central nervous system tissues. srGAP2 is expressed in zones of neuronal differentiation. It plays a role in the regeneration of neurons and axons. srGAP3, also called MEGAP (MEntal disorder associated GTPase-Activating Protein), is a Rho GAP with activity towards Rac1 and Cdc42. It impacts cell migration by regulating actin and microtubule cytoskeletal dynamics. The association between srGAP3 haploinsufficiency and mental retardation is under debate. srGAPs are Rho GAPs that interact with Robo1, the transmembrane receptor of Slit proteins. Slit proteins are secreted proteins that control axon guidance and the migration of neurons and leukocytes. srGAPs contain an N-terminal F-BAR domain, a Rho GAP domain, and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212888 [Multi-domain]  Cd Length: 53  Bit Score: 43.01  E-value: 2.36e-05
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11955      4 AKFDYVGRSARELSFKKGASLLLYHRASDDWWEGRHNGIDGLVPHQYI 51
SH3_SH3RF_3 cd11783
Third Src Homology 3 domain of SH3 domain containing ring finger 1 (SH3RF1), SH3RF3, and ...
1084-1131 2.66e-05

Third Src Homology 3 domain of SH3 domain containing ring finger 1 (SH3RF1), SH3RF3, and similar domains; SH3RF1 (or POSH) and SH3RF3 (or POSH2) are scaffold proteins that function as E3 ubiquitin-protein ligases. They contain an N-terminal RING finger domain and four SH3 domains. This model represents the third SH3 domain, located in the middle of SH3RF1 and SH3RF3, and similar domains. SH3RF1 plays a role in calcium homeostasis through the control of the ubiquitin domain protein Herp. It may also have a role in regulating death receptor mediated and JNK mediated apoptosis. SH3RF3 interacts with p21-activated kinase 2 (PAK2) and GTP-loaded Rac1. It may play a role in regulating JNK mediated apoptosis in certain conditions. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212717 [Multi-domain]  Cd Length: 55  Bit Score: 42.77  E-value: 2.66e-05
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGR--LHGQEGLFPGNYV 1131
Cdd:cd11783      4 ALYPYKPQKPDELELRKGEMYTVTEKCQDGWFKGTslRTGQSGVFPGNYV 53
SH3_PRMT2 cd11806
Src homology 3 domain of Protein arginine N-methyltransferase 2; PRMT2, also called HRMT1L1, ...
1082-1131 3.03e-05

Src homology 3 domain of Protein arginine N-methyltransferase 2; PRMT2, also called HRMT1L1, belongs to the arginine methyltransferase protein family. It functions as a coactivator to both estrogen receptor alpha (ER-alpha) and androgen receptor (AR), presumably through arginine methylation. The ER-alpha transcription factor is involved in cell proliferation, differentiation, morphogenesis, and apoptosis, and is also implicated in the development and progression of breast cancer. PRMT2 and its variants are upregulated in breast cancer cells and may be involved in modulating the ER-alpha signaling pathway during formation of breast cancer. PRMT2 also plays a role in regulating the function of E2F transcription factors, which are critical cell cycle regulators, by binding to the retinoblastoma gene product (RB). It contains an N-terminal SH3 domain and an AdoMet binding domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212740 [Multi-domain]  Cd Length: 53  Bit Score: 42.38  E-value: 3.03e-05
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gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11806      2 YVAIADFVATDDSQLSFESGDKLLVLRKPSVDWWWAEHNGCCGYIPASHL 51
SH3_DNMBP_N3 cd11796
Third N-terminal Src homology 3 domain of Dynamin Binding Protein, also called Tuba; DNMBP or ...
1081-1131 3.59e-05

Third N-terminal Src homology 3 domain of Dynamin Binding Protein, also called Tuba; DNMBP or Tuba is a cdc42-specific guanine nucleotide exchange factor (GEF) that contains four N-terminal SH3 domains, a central RhoGEF [or Dbl homology (DH)] domain followed by a Bin/Amphiphysin/Rvs (BAR) domain, and two C-terminal SH3 domains. It provides a functional link between dynamin and key regulatory proteins of the actin cytoskeleton. It plays an important role in regulating cell junction configuration. The four N-terminal SH3 domains of DNMBP binds the GTPase dynamin, which plays an important role in the fission of endocytic vesicles. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212730  Cd Length: 51  Bit Score: 42.34  E-value: 3.59e-05
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11796      1 QARVLQDLSAQLDEELDLREGDVVTITGILDKGWFRGELNGRRGIFPEGFV 51
SH3_ASAP2 cd11966
Src homology 3 domain of ArfGAP with SH3 domain, ankyrin repeat and PH domain containing ...
1081-1131 4.01e-05

Src homology 3 domain of ArfGAP with SH3 domain, ankyrin repeat and PH domain containing protein 2; ASAP2 is also called DDEF2 (Development and Differentiation Enhancing Factor 2), AMAP2, centaurin beta-3, or PAG3. It mediates the functions of Arf GTPases vial dual mechanisms: it exhibits GTPase activating protein (GAP) activity towards class I (Arf1) and II (Arf5) Arfs; and it binds class III Arfs (GTP-Arf6) stably without GAP activity. It binds paxillin and is implicated in Fcgamma receptor-mediated phagocytosis in macrophages and in cell migration. ASAP2 contains an N-terminal BAR domain, followed by a Pleckstrin homology (PH) domain, an Arf GAP domain, ankyrin (ANK) repeats, and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212899  Cd Length: 56  Bit Score: 42.25  E-value: 4.01e-05
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQ---EGLFPGNYV 1131
Cdd:cd11966      1 RVKALYNCVADNPDELTFSEGEIIIVDGEEDKEWWIGHIDGEptrRGAFPVSFV 54
SH3_Intersectin1_3 cd11991
Third Src homology 3 domain (or SH3C) of Intersectin-1; Intersectin-1 (ITSN1) is an adaptor ...
1084-1131 4.08e-05

Third Src homology 3 domain (or SH3C) of Intersectin-1; Intersectin-1 (ITSN1) is an adaptor protein that functions in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. It plays a role in clathrin-coated pit (CCP) formation. It binds to many proteins through its multidomain structure and facilitate the assembly of multimeric complexes. ITSN1 localizes in membranous organelles, CCPs, the Golgi complex, and may be involved in the cell membrane trafficking system. It exists in alternatively spliced short and long isoforms. The short isoform contains two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoform, in addition, contains RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. The third SH3 domain (or SH3C) of ITSN1 has been shown to bind many proteins including dynamin1/2, CIN85, c-Cbl, SHIP2, Reps1, synaptojanin-1, and WNK, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212924  Cd Length: 52  Bit Score: 42.28  E-value: 4.08e-05
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSgWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11991      4 AMYTYESNEQGDLTFQQGDVILVTKKDGD-WWTGTVGDKTGVFPSNYV 50
SH3_Noxa1_C cd12047
C-terminal Src Homology 3 domain of NADPH oxidase activator 1; Noxa1 is a homolog of p67phox ...
1081-1127 4.21e-05

C-terminal Src Homology 3 domain of NADPH oxidase activator 1; Noxa1 is a homolog of p67phox and is a cytosolic subunit of the nonphagocytic NADPH oxidase complex Nox1, which catalyzes the transfer of electrons from NADPH to molecular oxygen to form superoxide. Noxa1 is co-expressed with Nox1 in colon, stomach, uterus, prostate, and vascular smooth muscle cells, consistent with its regulatory role. It does not interact with p40phox, unlike p67phox, making Nox1 activity independent of p40phox, unlike Nox2. Noxa1 contains TPR, PB1, and C-terminal SH3 domains, but lacks the central SH3 domain that is present in p67phox. The TPR domain binds activated GTP-bound Rac. The C-terminal SH3 domain binds the polyproline motif found at the C-terminus of Noxo1, a homolog of p47phox. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212980  Cd Length: 53  Bit Score: 42.11  E-value: 4.21e-05
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFP 1127
Cdd:cd12047      1 RMVAQHDYSAQGPEDLEFSQGDTIDILSEVNQEWLEGHCDGRIGIFP 47
SH3_Abp1_fungi_C1 cd11962
First C-terminal Src homology 3 domain of Fungal Actin-binding protein 1; Abp1 is an adaptor ...
1081-1132 4.56e-05

First C-terminal Src homology 3 domain of Fungal Actin-binding protein 1; Abp1 is an adaptor protein that functions in receptor-mediated endocytosis and vesicle trafficking. It contains an N-terminal actin-binding module, the actin-depolymerizing factor (ADF) homology domain, a central proline-rich region, and a C-terminal SH3 domain (many yeast Abp1 proteins contain two C-terminal SH3 domains). Yeast Abp1 also contains two acidic domains that bind directly to the Arp2/3 complex, which is required to initiate actin polymerization. The SH3 domain of yeast Abp1 binds and localizes the kinases, Ark1p and Prk1p, which facilitate actin patch disassembly following vesicle internalization. It also mediates the localization to the actin patch of the synaptojanin-like protein, Sjl2p, which plays a key role in endocytosis. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212895 [Multi-domain]  Cd Length: 54  Bit Score: 42.09  E-value: 4.56e-05
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKG-RLHGQEGLFPGNYVE 1132
Cdd:cd11962      1 RAVVLYDYEKDEDNEIELVEGEIVTNIEMVDEDWWMGtNSKGESGLFPSNYVE 53
SH3_SH3RF3_3 cd11925
Third Src Homology 3 domain of SH3 domain containing ring finger 3, an E3 ubiquitin-protein ...
1084-1134 4.59e-05

Third Src Homology 3 domain of SH3 domain containing ring finger 3, an E3 ubiquitin-protein ligase; SH3RF3 is also called POSH2 (Plenty of SH3s 2) or SH3MD4 (SH3 multiple domains protein 4). It is a scaffold protein with E3 ubiquitin-protein ligase activity. It was identified in the screen for interacting partners of p21-activated kinase 2 (PAK2). It may play a role in regulating JNK mediated apoptosis in certain conditions. It also interacts with GTP-loaded Rac1. SH3RF3 is highly homologous to SH3RF1; it also contains an N-terminal RING finger domain and four SH3 domains. This model represents the third SH3 domain, located in the middle, of SH3RF3. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212858  Cd Length: 57  Bit Score: 42.29  E-value: 4.59e-05
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGR--LHGQEGLFPGNYVEKI 1134
Cdd:cd11925      5 ALYAYKPQKNDELELRKGEMYRVIEKCQDGWFKGTslRTGVSGVFPGNYVTPV 57
SH3_Fyn_Yrk cd12006
Src homology 3 domain of Fyn and Yrk Protein Tyrosine Kinases; Fyn and Yrk (Yes-related kinase) ...
1084-1131 5.05e-05

Src homology 3 domain of Fyn and Yrk Protein Tyrosine Kinases; Fyn and Yrk (Yes-related kinase) are members of the Src subfamily of proteins, which are cytoplasmic (or non-receptor) PTKs. Fyn, together with Lck, plays a critical role in T-cell signal transduction by phosphorylating ITAM (immunoreceptor tyr activation motif) sequences on T-cell receptors, ultimately leading to the proliferation and differentiation of T-cells. In addition, Fyn is involved in the myelination of neurons, and is implicated in Alzheimer's and Parkinson's diseases. Yrk has been detected only in chickens. It is primarily found in neuronal and epithelial cells and in macrophages. It may play a role in inflammation and in response to injury. Src kinases contain an N-terminal SH4 domain with a myristoylation site, followed by SH3 and SH2 domains, a tyr kinase domain, and a regulatory C-terminal region containing a conserved tyr. They are activated by autophosphorylation at the tyr kinase domain, but are negatively regulated by phosphorylation at the C-terminal tyr by Csk (C-terminal Src Kinase). The SH3 domain of Src kinases contributes to substrate recruitment by binding adaptor proteins/substrates, and regulation of kinase activity through an intramolecular interaction. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212939 [Multi-domain]  Cd Length: 56  Bit Score: 41.96  E-value: 5.05e-05
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGR--LHGQEGLFPGNYV 1131
Cdd:cd12006      5 ALYDYEARTEDDLSFHKGEKFQILNSSEGDWWEARslTTGETGYIPSNYV 54
SH3_CIP4_Bzz1_like cd11777
Src Homology 3 domain of Cdc42-Interacting Protein 4, Bzz1 and similar domains; This subfamily ...
1082-1131 5.29e-05

Src Homology 3 domain of Cdc42-Interacting Protein 4, Bzz1 and similar domains; This subfamily is composed of Cdc42-Interacting Protein 4 (CIP4) and similar proteins such as Formin Binding Protein 17 (FBP17) and FormiN Binding Protein 1-Like (FNBP1L), as well as yeast Bzz1 (or Bzz1p). CIP4 and FNBP1L are Cdc42 effectors that bind Wiskott-Aldrich syndrome protein (WASP) and function in endocytosis. CIP4 and FBP17 bind to the Fas ligand and may be implicated in the inflammatory response. CIP4 may also play a role in phagocytosis. Bzz1 is also a WASP/Las17-interacting protein involved in endocytosis and trafficking to the vacuole. It physically interacts with type I myosins and functions in the early steps of endocytosis. Members of this subfamily contain an N-terminal F-BAR (FES-CIP4 Homology and Bin/Amphiphysin/Rvs) domain as well as at least one C-terminal SH3 domain. Bzz1 contains a second SH3 domain at the C-terminus. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212711 [Multi-domain]  Cd Length: 55  Bit Score: 41.83  E-value: 5.29e-05
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gi 1622892340 1082 CRALYQYVGQDVDELSFNVNEVIEILMEDS-SGWWK-GRLHGQEGLFPGNYV 1131
Cdd:cd11777      2 CKALYAFVGSSEGTISMTEGEKLSLVEEDKgDGWTRvRRDTGEEGYVPTSYI 53
SH3_BOI cd11886
Src Homology 3 domain of fungal BOI-like proteins; This subfamily includes the Saccharomyces ...
1083-1130 5.58e-05

Src Homology 3 domain of fungal BOI-like proteins; This subfamily includes the Saccharomyces cerevisiae proteins BOI1 and BOI2, and similar proteins. They contain an N-terminal SH3 domain, a Sterile alpha motif (SAM), and a Pleckstrin homology (PH) domain at the C-terminus. BOI1 and BOI2 interact with the SH3 domain of Bem1p, a protein involved in bud formation. They promote polarized cell growth and participates in the NoCut signaling pathway, which is involved in the control of cytokinesis. SH3 domains bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs; they play a role in the regulation of enzymes by intramolecular interactions, changing the subcellular localization of signal pathway components and mediate multiprotein complex assemblies.


Pssm-ID: 212819  Cd Length: 55  Bit Score: 41.93  E-value: 5.58e-05
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDS---SGWWKGR--LHGQEGLFPGNY 1130
Cdd:cd11886      3 IVIHDFNARSEDELTLKPGDKIELIEDDEefgDGWYLGRnlRTGETGLFPVVF 55
SH3_Nephrocystin cd11770
Src Homology 3 domain of Nephrocystin (or Nephrocystin-1); Nephrocystin contains an SH3 domain ...
1081-1133 5.74e-05

Src Homology 3 domain of Nephrocystin (or Nephrocystin-1); Nephrocystin contains an SH3 domain involved in signaling pathways that regulate cell adhesion and cytoskeletal organization. It is a protein that in humans is associated with juvenile nephronophthisis, an inherited kidney disease characterized by renal fibrosis that lead to chronic renal failure in children. It is localized in cell-cell junctions in renal duct cells, and is known to interact with Ack1, an activated Cdc42-associated kinase. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212704 [Multi-domain]  Cd Length: 54  Bit Score: 41.91  E-value: 5.74e-05
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKG-RLHGQEGLFPGNYVEK 1133
Cdd:cd11770      1 LYEALSDFQAEQEGDLSFKKGEVLRIISKRADGWWLAeNSKGNRGLVPKTYLKV 54
SH3_Intersectin1_1 cd11987
First Src homology 3 domain (or SH3A) of Intersectin-1; Intersectin-1 (ITSN1) is an adaptor ...
1083-1133 6.14e-05

First Src homology 3 domain (or SH3A) of Intersectin-1; Intersectin-1 (ITSN1) is an adaptor protein that functions in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. It plays a role in clathrin-coated pit (CCP) formation. It binds to many proteins through its multidomain structure and facilitate the assembly of multimeric complexes. ITSN1 localizes in membranous organelles, CCPs, the Golgi complex, and may be involved in the cell membrane trafficking system. It exists in alternatively spliced short and long isoforms. The short isoform contains two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoform, in addition, contains RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. The first SH3 domain (or SH3A) of ITSN1 has been shown to bind many proteins including Sos1, dynamin1/2, CIN85, c-Cbl, PI3K-C2, SHIP2, N-WASP, and CdGAP, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212920 [Multi-domain]  Cd Length: 55  Bit Score: 41.91  E-value: 6.14e-05
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSS--GWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11987      3 RALYPFEARSHDEITIQPGDIVMVDESQTGepGWLGGELKGKTGWFPANYAEK 55
SH3_MYO15 cd11884
Src Homology 3 domain of Myosin XV; This subfamily is composed of proteins with similarity to ...
1083-1132 6.48e-05

Src Homology 3 domain of Myosin XV; This subfamily is composed of proteins with similarity to Myosin XVa. Myosin XVa is an unconventional myosin that is critical for the normal growth of mechanosensory stereocilia of inner ear hair cells. Mutations in the myosin XVa gene are associated with nonsyndromic hearing loss. Myosin XVa contains a unique N-terminal extension followed by a motor domain, light chain-binding IQ motifs, and a tail consisting of a pair of MyTH4-FERM tandems separated by a SH3 domain, and a PDZ domain. SH3 domains bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs; they play a role in the regulation of enzymes by intramolecular interactions, changing the subcellular localization of signal pathway components and mediate multiprotein complex assemblies.


Pssm-ID: 212817 [Multi-domain]  Cd Length: 56  Bit Score: 41.54  E-value: 6.48e-05
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEIL---MEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11884      3 VAVRAYITRDQTLLSFHKGDVIKLLpkeGPLDPGWLFGTLDGRSGAFPKEYVQ 55
SH3_VAV2_2 cd11977
C-terminal (or second) Src homology 3 domain of VAV2 protein; VAV2 is widely expressed and ...
1084-1133 6.70e-05

C-terminal (or second) Src homology 3 domain of VAV2 protein; VAV2 is widely expressed and functions as a guanine nucleotide exchange factor (GEF) for RhoA, RhoB and RhoG and also activates Rac1 and Cdc42. It is implicated in many cellular and physiological functions including blood pressure control, eye development, neurite outgrowth and branching, EGFR endocytosis and degradation, and cell cluster morphology, among others. It has been reported to associate with Nek3. VAV proteins contain several domains that enable their function: N-terminal calponin homology (CH), acidic, RhoGEF (also called Dbl-homologous or DH), Pleckstrin Homology (PH), C1 (zinc finger), SH2, and two SH3 domains. The SH3 domain of VAV is involved in the localization of proteins to specific sites within the cell, by interacting with proline-rich sequences within target proteins. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212910 [Multi-domain]  Cd Length: 58  Bit Score: 41.54  E-value: 6.70e-05
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEIL--MEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11977      5 ARYNFAARDMRELSLREGDVVRIYsrIGGDQGWWKGETNGRIGWFPSTYVEE 56
SH3_Bbc1 cd11887
Src Homology 3 domain of Bbc1 and similar domains; This subfamily is composed of Saccharomyces ...
1081-1133 7.98e-05

Src Homology 3 domain of Bbc1 and similar domains; This subfamily is composed of Saccharomyces cerevisiae Bbc1p, also called Mti1p (Myosin tail region-interacting protein), and similar proteins. Bbc1p interacts with and regulates type I myosins in yeast, Myo3p and Myo5p, which are involved in actin cytoskeletal reorganization. It also binds and inhibits Las17, a WASp family protein that functions as an activator of the Arp2/3 complex. Bbc1p contains an N-terminal SH3 domain. SH3 domains bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs; they play a role in the regulation of enzymes by intramolecular interactions, changing the subcellular localization of signal pathway components and mediate multiprotein complex assemblies.


Pssm-ID: 212820 [Multi-domain]  Cd Length: 60  Bit Score: 41.56  E-value: 7.98e-05
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRL---HG--QEGLFPGNYVEK 1133
Cdd:cd11887      3 KVKALYPYESDHEDDLNFDVGQLITVTEEEDADWYFGEYvdsNGntKEGIFPKNFVEV 60
SH3_Yes cd12007
Src homology 3 domain of Yes Protein Tyrosine Kinase; Yes (or c-Yes) is a member of the Src ...
1084-1131 8.69e-05

Src homology 3 domain of Yes Protein Tyrosine Kinase; Yes (or c-Yes) is a member of the Src subfamily of proteins, which are cytoplasmic (or non-receptor) PTKs. c-Yes kinase is the cellular homolog of the oncogenic protein (v-Yes) encoded by the Yamaguchi 73 and Esh sarcoma viruses. It displays functional overlap with other Src subfamily members, particularly Src. It also shows some unique functions such as binding to occludins, transmembrane proteins that regulate extracellular interactions in tight junctions. Yes also associates with a number of proteins in different cell types that Src does not interact with, like JAK2 and gp130 in pre-adipocytes, and Pyk2 in treated pulmonary vein endothelial cells. Although the biological function of Yes remains unclear, it appears to have a role in regulating cell-cell interactions and vesicle trafficking in polarized cells. Src kinases contain an N-terminal SH4 domain with a myristoylation site, followed by SH3 and SH2 domains, a tyr kinase domain, and a regulatory C-terminal region containing a conserved tyr. They are activated by autophosphorylation at the tyr kinase domain, but are negatively regulated by phosphorylation at the C-terminal tyr by Csk (C-terminal Src Kinase). The SH3 domain of Src kinases contributes to substrate recruitment by binding adaptor proteins/substrates, and regulation of kinase activity through an intramolecular interaction. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212940 [Multi-domain]  Cd Length: 58  Bit Score: 41.56  E-value: 8.69e-05
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGR--LHGQEGLFPGNYV 1131
Cdd:cd12007      5 ALYDYEARTTEDLSFKKGERFQIINNTEGDWWEARsiATGKNGYIPSNYV 54
SH3_GRAF cd12064
Src Homology 3 domain of GTPase Regulator Associated with Focal adhesion kinase; GRAF, also ...
1081-1132 9.51e-05

Src Homology 3 domain of GTPase Regulator Associated with Focal adhesion kinase; GRAF, also called Rho GTPase activating protein 26 (ARHGAP26), Oligophrenin-1-like (OPHN1L) or GRAF1, is a GAP with activity towards RhoA and Cdc42 and is only weakly active towards Rac1. It influences Rho-mediated cytoskeletal rearrangements and binds focal adhesion kinase (FAK), which is a critical component of integrin signaling. It is essential for the major clathrin-independent endocytic pathway mediated by pleiomorphic membranes. GRAF contains an N-terminal BAR domain, followed by a Pleckstrin homology (PH) domain, a Rho GAP domain, and a C-terminal SH3 domain. The SH3 domain of GRAF binds PKNbeta, a target of the small GTPase Rho. SH3 domains bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs; they play a role in the regulation of enzymes by intramolecular interactions, changing the subcellular localization of signal pathway components and mediate multiprotein complex assemblies.


Pssm-ID: 212997  Cd Length: 56  Bit Score: 41.25  E-value: 9.51e-05
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIE-ILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd12064      2 KAKALYACKAEHDSELSFTAGTVFDnVHPSQEPGWLEGTLNGKTGLIPENYVE 54
SH3_SKAP2 cd12045
Src Homology 3 domain of Src Kinase-Associated Phosphoprotein 2; SKAP2, also called ...
1083-1131 9.72e-05

Src Homology 3 domain of Src Kinase-Associated Phosphoprotein 2; SKAP2, also called SKAP55-Related (SKAP55R) or SKAP55 homolog (SKAP-HOM or SKAP55-HOM), is an immune cell-specific adaptor protein that plays an important role in adhesion and migration of B-cells and macrophages. Binding partners include ADAP (adhesion and degranulation-promoting adaptor protein), YopH, SHPS1, and HPK1. SKAP2 has also been identified as a substrate for lymphoid-specific tyrosine phosphatase (Lyp), which has been implicated in a wide variety of autoimmune diseases. It contains a pleckstrin homology (PH) domain, a C-terminal SH3 domain, and several tyrosine phosphorylation sites. Like SKAP1, SKAP2 is expected to bind primarily to a proline-rich region of ADAP through its SH3 domain; its degradation may be regulated by ADAP. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212978  Cd Length: 53  Bit Score: 41.04  E-value: 9.72e-05
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILME--DSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd12045      3 QGLWDCTGDQPDELSFKRGDTIYILSKeyNRFGWWVGEMKGTIGLVPKAYI 53
SH3_Stac3_1 cd11986
First C-terminal Src homology 3 domain of SH3 and cysteine-rich domain-containing protein 3 ...
1084-1131 1.10e-04

First C-terminal Src homology 3 domain of SH3 and cysteine-rich domain-containing protein 3 (Stac3); Stac proteins are putative adaptor proteins that contain a cysteine-rich C1 domain and one or two SH3 domains at the C-terminus. There are three mammalian members (Stac1, Stac2, and Stac3) of this family. Stac1 and Stac3 contain two SH3 domains while Stac2 contains a single SH3 domain at the C-terminus. Stac1 and Stac2 have been found to be expressed differently in mature dorsal root ganglia (DRG) neurons. Stac1 is mainly expressed in peptidergic neurons while Stac2 is found in a subset of nonpeptidergic and all trkB+ neurons. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212919 [Multi-domain]  Cd Length: 53  Bit Score: 41.05  E-value: 1.10e-04
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11986      4 ALYRFKALEKDDLDFHPGERITVIDDSNEEWWRGKIGEKTGYFPMNFI 51
SH3_Eps8 cd11764
Src Homology 3 domain of Epidermal growth factor receptor kinase substrate 8 and similar ...
1083-1132 1.21e-04

Src Homology 3 domain of Epidermal growth factor receptor kinase substrate 8 and similar proteins; This group is composed of Eps8 and Eps8-like proteins including Eps8-like 1-3, among others. These proteins contain N-terminal Phosphotyrosine-binding (PTB), central SH3, and C-terminal effector domains. Eps8 binds either Abi1 (also called E3b1) or Rab5 GTPase activating protein RN-tre through its SH3 domain. With Abi1 and Sos1, it becomes part of a trimeric complex that is required to activate Rac. Together with RN-tre, it inhibits the internalization of EGFR. The SH3 domains of Eps8 and similar proteins recognize peptides containing a PxxDY motif, instead of the classical PxxP motif. SH3 domains are protein interaction domains that usually bind to proline-rich ligands with moderate affinity and selectivity. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212698 [Multi-domain]  Cd Length: 54  Bit Score: 40.71  E-value: 1.21e-04
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILmEDSSGWWKGR-LHGQEGLFPGNYVE 1132
Cdd:cd11764      3 RVLYDFTARNSKELSVLKGEYLEVL-DDSRQWWKVRnSRGQVGYVPHNILE 52
SH3_Tks_3 cd12017
Third Src homology 3 domain of Tyrosine kinase substrate (Tks) proteins; Tks proteins are Src ...
1094-1133 1.36e-04

Third Src homology 3 domain of Tyrosine kinase substrate (Tks) proteins; Tks proteins are Src substrates and scaffolding proteins that play important roles in the formation of podosomes and invadopodia, the dynamic actin-rich structures that are related to cell migration and cancer cell invasion. Vertebrates contain two Tks proteins, Tks4 (Tyr kinase substrate with four SH3 domains) and Tks5 (Tyr kinase substrate with five SH3 domains), which display partially overlapping but non-redundant functions. Both associate with the ADAMs family of transmembrane metalloproteases, which function as sheddases and mediators of cell and matrix interactions. Tks5 interacts with N-WASP and Nck, while Tks4 is essential for the localization of MT1-MMP (membrane-type 1 matrix metalloproteinase) to invadopodia. Tks proteins contain an N-terminal Phox homology (PX) domain and four or five SH3 domains. This model characterizes the third SH3 domain of Tks proteins. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212950  Cd Length: 53  Bit Score: 40.51  E-value: 1.36e-04
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gi 1622892340 1094 DELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd12017     14 DGISFQKGQKVEVIDKNPSGWWYVKIDGKEGWAPSSYIEK 53
SH3_RIM-BP_3 cd12013
Third Src homology 3 domain of Rab3-interacting molecules (RIMs) binding proteins; RIMs ...
1081-1132 1.65e-04

Third Src homology 3 domain of Rab3-interacting molecules (RIMs) binding proteins; RIMs binding proteins (RBPs, RIM-BPs) associate with calcium channels present in photoreceptors, neurons, and hair cells; they interact simultaneously with specific calcium channel subunits, and active zone proteins, RIM1 and RIM2. RIMs are part of the matrix at the presynaptic active zone and are associated with synaptic vesicles through their interaction with the small GTPase Rab3. RIM-BPs play a role in regulating synaptic transmission by serving as adaptors and linking calcium channels with the synaptic vesicle release machinery. RIM-BPs contain three SH3 domains and two to three fibronectin III repeats. Invertebrates contain one, while vertebrates contain at least two RIM-BPs, RIM-BP1 and RIM-BP2. RIM-BP1 is also called peripheral-type benzodiazapine receptor associated protein 1 (PRAX-1). Mammals contain a third protein, RIM-BP3. RIM-BP1 and RIM-BP2 are predominantly expressed in the brain where they display overlapping but distinct expression patterns, while RIM-BP3 is almost exclusively expressed in the testis and is essential in spermiogenesis. The SH3 domains of RIM-BPs bind to the PxxP motifs of RIM1, RIM2, and L-type (alpha1D) and N-type (alpha1B) calcium channel subunits. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212946  Cd Length: 61  Bit Score: 40.83  E-value: 1.65e-04
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gi 1622892340 1081 RCRALYQYVGQ------DVD-ELSFNVNEVIEILME-DSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd12013      1 RMVALFDYDPResspnvDAEvELSFRAGDIITVFGEmDEDGFYYGELNGQRGLVPSNFLE 60
SH3_TXK cd11907
Src Homology 3 domain of TXK, also called Resting lymphocyte kinase (Rlk); TXK is a ...
1081-1131 1.66e-04

Src Homology 3 domain of TXK, also called Resting lymphocyte kinase (Rlk); TXK is a cytoplasmic (or nonreceptor) tyr kinase containing Src homology protein interaction domains (SH3, SH2) N-terminal to the catalytic tyr kinase domain. It also contains an N-terminal cysteine-rich region. Rlk is expressed in T-cells and mast cell lines, and is a key component of T-cell receptor (TCR) signaling. It is important in TCR-stimulated proliferation, IL-2 production and phospholipase C-gamma1 activation. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212840 [Multi-domain]  Cd Length: 55  Bit Score: 40.32  E-value: 1.66e-04
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLH-GQEGLFPGNYV 1131
Cdd:cd11907      2 QVKALYDFLPREPSNLALKRAEEYLILEQYDPHWWKARDRyGNEGLIPSNYV 53
SH3_p67phox_C cd12046
C-terminal (or second) Src Homology 3 domain of the p67phox subunit of NADPH oxidase; p67phox, ...
1084-1132 1.74e-04

C-terminal (or second) Src Homology 3 domain of the p67phox subunit of NADPH oxidase; p67phox, also called Neutrophil cytosol factor 2 (NCF-2), is a cytosolic subunit of the phagocytic NADPH oxidase complex (also called Nox2 or gp91phox) which plays a crucial role in the cellular response to bacterial infection. NADPH oxidase catalyzes the transfer of electrons from NADPH to oxygen during phagocytosis forming superoxide and reactive oxygen species. p67phox plays a regulatory role and contains N-terminal TPR, first SH3 (or N-terminal or central SH3), PB1, and C-terminal SH3 domains. It binds, via its C-terminal SH3 domain, to a proline-rich region of p47phox and upon activation, this complex assembles with flavocytochrome b558, the Nox2-p22phox heterodimer. Concurrently, RacGTP translocates to the membrane and interacts with the TPR domain of p67phox, which leads to the activation of NADPH oxidase. The PB1 domain of p67phox binds to its partner PB1 domain in p40phox, and this facilitates the assembly of p47phox-p67phox at the membrane. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212979 [Multi-domain]  Cd Length: 53  Bit Score: 40.56  E-value: 1.74e-04
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd12046      4 ALFSYEASQPEDLEFQKGDVILVLSKVNEDWLEGQCKGKIGIFPSAFVE 52
SH3_ARHGAP32_33 cd11835
Src homology 3 domain of Rho GTPase-activating proteins 32 and 33, and similar proteins; ...
1088-1131 1.75e-04

Src homology 3 domain of Rho GTPase-activating proteins 32 and 33, and similar proteins; Members of this family contain N-terminal PX and Src Homology 3 (SH3) domains, a central Rho GAP domain, and C-terminal extensions. RhoGAPs (or ARHGAPs) bind to Rho proteins and enhance the hydrolysis rates of bound GTP. ARHGAP32 is also called RICS, PX-RICS, p250GAP, or p200RhoGAP. It is a Rho GTPase-activating protein for Cdc42 and Rac1, and is implicated in the regulation of postsynaptic signaling and neurite outgrowth. PX-RICS, a variant of RICS that contain PX and SH3 domains, is the main isoform expressed during neural development. It is involved in neural functions including axon and dendrite extension, postnatal remodeling, and fine-tuning of neural circuits during early brain development. ARHGAP33, also called sorting nexin 26 or TCGAP (Tc10/CDC42 GTPase-activating protein), is widely expressed in the brain where it is involved in regulating the outgrowth of axons and dendrites and is regulated by the protein tyrosine kinase Fyn. It is translocated to the plasma membrane in adipocytes in response to insulin and may be involved in the regulation of insulin-stimulated glucose transport. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212769 [Multi-domain]  Cd Length: 54  Bit Score: 40.51  E-value: 1.75e-04
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gi 1622892340 1088 YVGQDVDELSFNVNEVIEIL----MEDSSgWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11835      8 YTAQAPDELSLEVGDIVSVIdmppPEEST-WWRGKKGFQVGFFPSECV 54
SH3_SKAP1-like cd11866
Src Homology 3 domain of Src Kinase-Associated Phosphoprotein 1 and similar proteins; This ...
1083-1131 1.78e-04

Src Homology 3 domain of Src Kinase-Associated Phosphoprotein 1 and similar proteins; This subfamily is composed of SKAP1, SKAP2, and similar proteins. SKAP1 and SKAP2 are immune cell-specific adaptor proteins that play roles in T- and B-cell adhesion, respectively, and are thus important in the migration of T- and B-cells to sites of inflammation and for movement during T-cell conjugation with antigen-presenting cells. Both SKAP1 and SKAP2 bind to ADAP (adhesion and degranulation-promoting adaptor protein), among many other binding partners. They contain a pleckstrin homology (PH) domain, a C-terminal SH3 domain, and several tyrosine phosphorylation sites. The SH3 domain of SKAP1 is necessary for its ability to regulate T-cell conjugation with antigen-presenting cells and the formation of LFA-1 clusters. SKAP1 binds primarily to a proline-rich region of ADAP through its SH3 domain; its degradation is regulated by ADAP. A secondary interaction occurs via the ADAP SH3 domain and the RKxxYxxY motif in SKAP1. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212800  Cd Length: 53  Bit Score: 40.49  E-value: 1.78e-04
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILME--DSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11866      3 MGLWDCSGNEPDELSFKRGDLIYIISKeyDSFGWWVGELNGKVGLVPKDYL 53
SH3_UBASH3A cd11937
Src homology 3 domain of Ubiquitin-associated and SH3 domain-containing protein A; UBASH3A is ...
1083-1133 2.05e-04

Src homology 3 domain of Ubiquitin-associated and SH3 domain-containing protein A; UBASH3A is also called Cbl-Interacting Protein 4 (CLIP4), T cell Ubiquitin LigAnd (TULA), or T cell receptor Signaling (STS)-2. It is only found in lymphoid cells and exhibits weak phosphatase activity. UBASH3A facilitates T cell-induced apoptosis through interaction with the apoptosis-inducing factor AIF. It is involved in regulating the level of phosphorylation of the zeta-associated protein (ZAP)-70 tyrosine kinase. TULA proteins contain an N-terminal UBA domain, a central SH3 domain, and a C-terminal histidine phosphatase domain. They bind c-Cbl through the SH3 domain and to ubiquitin via UBA. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212870 [Multi-domain]  Cd Length: 60  Bit Score: 40.39  E-value: 2.05e-04
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEI----LMEDSSGWWKGRLH--GQEGLFPGNYVEK 1133
Cdd:cd11937      4 RALFQYKPQNIDELMLSPGDYIFVdptqQSEASEGWVIGISHrtGCRGFLPENYTER 60
SH3_Tks_1 cd12015
First Src homology 3 domain of Tyrosine kinase substrate (Tks) proteins; Tks proteins are Src ...
1088-1133 2.10e-04

First Src homology 3 domain of Tyrosine kinase substrate (Tks) proteins; Tks proteins are Src substrates and scaffolding proteins that play important roles in the formation of podosomes and invadopodia, the dynamic actin-rich structures that are related to cell migration and cancer cell invasion. Vertebrates contain two Tks proteins, Tks4 (Tyr kinase substrate with four SH3 domains) and Tks5 (Tyr kinase substrate with five SH3 domains), which display partially overlapping but non-redundant functions. Both associate with the ADAMs family of transmembrane metalloproteases, which function as sheddases and mediators of cell and matrix interactions. Tks5 interacts with N-WASP and Nck, while Tks4 is essential for the localization of MT1-MMP (membrane-type 1 matrix metalloproteinase) to invadopodia. Tks proteins contain an N-terminal Phox homology (PX) domain and four or five SH3 domains. This model characterizes the first SH3 domain of Tks proteins. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212948  Cd Length: 53  Bit Score: 40.10  E-value: 2.10e-04
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gi 1622892340 1088 YVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd12015      8 YKKQQPNEISLRAGDVVDVIEKNENGWWFVSLEDEQGWVPATYLEP 53
PHA03247 PHA03247
large tegument protein UL36; Provisional
948-1085 2.53e-04

large tegument protein UL36; Provisional


Pssm-ID: 223021 [Multi-domain]  Cd Length: 3151  Bit Score: 45.70  E-value: 2.53e-04
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gi 1622892340  948 DGLPKSSKPTRKGMAKGRPRRSsqaptraaptrAAPGPPRGMDRNGVPPSARGGPLPLEIMSGGSSHRPPRGPPSTslgA 1027
Cdd:PHA03247  2590 DAPPQSARPRAPVDDRGDPRGP-----------APPSPLPPDTHAPDPPPPSPSPAANEPDPHPPPTVPPPERPRD---D 2655
                           90       100       110       120       130       140
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gi 1622892340 1028 SRRPRAQLPseHNTEFLNVPDQGMAGMQRKRSVGQRP----VPGVGRPKPQPRTHGPRCRAL 1085
Cdd:PHA03247  2656 PAPGRVSRP--RRARRLGRAAQASSPPQRPRRRAARPtvgsLTSLADPPPPPPTPEPAPHAL 2715
SH3_ASPP2 cd11953
Src Homology 3 (SH3) domain of Apoptosis Stimulating of p53 protein 2; ASPP2 is the full ...
1084-1129 2.73e-04

Src Homology 3 (SH3) domain of Apoptosis Stimulating of p53 protein 2; ASPP2 is the full length form of the previously-identified tumor supressor, p53-binding protein 2 (p53BP2). ASPP2 activates the apoptotic function of the p53 family of tumor suppressors (p53, p63, and p73). It plays a central role in regulating apoptosis and cell growth; ASPP2-deficient mice show postnatal death. Downregulated expression of ASPP2 is frequently found in breast tumors, lung cancer, and diffuse large B-cell lymphoma where it is correlated with a poor clinical outcome. ASPP2 contains a proline-rich region, four ankyrin (ANK) repeats, and an SH3 domain at its C-terminal half. The SH3 domain and the ANK repeats of ASPP2 contribute to the p53 binding site; they bind to the DNA binding domain of p53. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212886 [Multi-domain]  Cd Length: 57  Bit Score: 39.93  E-value: 2.73e-04
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILM---EDSSGWWKGRLHGQEGLFPGN 1129
Cdd:cd11953      5 ALWDYEGESDDELSFKEGDCMTILRredEDETEWWWARLNDKEGYVPRN 53
SH3_SH3RF2_3 cd11784
Third Src Homology 3 domain of SH3 domain containing ring finger 2; SH3RF2 is also called ...
1081-1131 2.78e-04

Third Src Homology 3 domain of SH3 domain containing ring finger 2; SH3RF2 is also called POSHER (POSH-eliminating RING protein) or HEPP1 (heart protein phosphatase 1-binding protein). It acts as an anti-apoptotic regulator of the JNK pathway by binding to and promoting the degradation of SH3RF1 (or POSH), a scaffold protein that is required for pro-apoptotic JNK activation. It may also play a role in cardiac functions together with protein phosphatase 1. SH3RF2 contains an N-terminal RING finger domain and three SH3 domains. This model represents the third SH3 domain, located in the middle, of SH3RF2. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212718  Cd Length: 55  Bit Score: 39.76  E-value: 2.78e-04
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGR--LHGQEGLFPGNYV 1131
Cdd:cd11784      1 MCVALHSYSAHRPEELELQKGEGVRVLGKFQEGWLRGLslVTGRVGIFPSNYV 53
SH3_Nck_1 cd11765
First Src Homology 3 domain of Nck adaptor proteins; Nck adaptor proteins regulate actin ...
1084-1131 2.85e-04

First Src Homology 3 domain of Nck adaptor proteins; Nck adaptor proteins regulate actin cytoskeleton dynamics by linking proline-rich effector molecules to protein tyrosine kinases and phosphorylated signaling intermediates. They contain three SH3 domains and a C-terminal SH2 domain. They function downstream of the PDGFbeta receptor and are involved in Rho GTPase signaling and actin dynamics. Vertebrates contain two Nck adaptor proteins: Nck1 (also called Nckalpha) and Nck2 (also called Nckbeta or Growth factor receptor-bound protein 4, Grb4), which show partly overlapping functions but also bind distinct targets. Their SH3 domains are involved in recruiting downstream effector molecules, such as the N-WASP/Arp2/3 complex, which when activated induces actin polymerization that results in the production of pedestals, or protrusions of the plasma membrane. The first SH3 domain of Nck proteins preferentially binds the PxxDY sequence, which is present in the CD3e cytoplasmic tail. This binding inhibits phosphorylation by Src kinases, resulting in the downregulation of TCR surface expression. SH3 domains are protein interaction domains that usually bind to proline-rich ligands with moderate affinity and selectivity, preferentially a PxxP motif. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212699 [Multi-domain]  Cd Length: 51  Bit Score: 39.71  E-value: 2.85e-04
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIeILMEDSSGWWKGR-LHGQEGLFPGNYV 1131
Cdd:cd11765      4 AKYDYTAQGDQELSIKKNEKL-TLLDDSKHWWKVQnSSNQTGYVPSNYV 51
SH3_SH3RF_C cd11785
C-terminal (Fourth) Src Homology 3 domain of SH3 domain containing ring finger 1 (SH3RF1), ...
1081-1133 2.99e-04

C-terminal (Fourth) Src Homology 3 domain of SH3 domain containing ring finger 1 (SH3RF1), SH3RF3, and similar domains; SH3RF1 (or POSH) and SH3RF3 (or POSH2) are scaffold proteins that function as E3 ubiquitin-protein ligases. They contain an N-terminal RING finger domain and four SH3 domains. This model represents the fourth SH3 domain, located at the C-terminus of SH3RF1 and SH3RF3, and similar domains. SH3RF1 plays a role in calcium homeostasis through the control of the ubiquitin domain protein Herp. It may also have a role in regulating death receptor mediated and JNK mediated apoptosis. SH3RF3 interacts with p21-activated kinase 2 (PAK2) and GTP-loaded Rac1. It may play a role in regulating JNK mediated apoptosis in certain conditions. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212719  Cd Length: 55  Bit Score: 39.76  E-value: 2.99e-04
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLH--GQEGLFPGNYVEK 1133
Cdd:cd11785      1 RYRVIVPYPPQSEAELELKEGDIVFVHKKREDGWFKGTLQrtGKTGLFPGSFVES 55
SH3_CRK_C cd11759
C-terminal Src Homology 3 domain of Ct10 Regulator of Kinase adaptor proteins; CRK adaptor ...
1092-1132 3.13e-04

C-terminal Src Homology 3 domain of Ct10 Regulator of Kinase adaptor proteins; CRK adaptor proteins consists of SH2 and SH3 domains, which bind tyrosine-phosphorylated peptides and proline-rich motifs, respectively. They function downstream of protein tyrosine kinases in many signaling pathways started by various extracellular signals, including growth and differentiation factors. Cellular CRK (c-CRK) contains a single SH2 domain, followed by N-terminal and C-terminal SH3 domains. It is involved in the regulation of many cellular processes including cell growth, motility, adhesion, and apoptosis. CRK has been implicated in the malignancy of various human cancers. The C-terminal SH3 domain of CRK has not been shown to bind any target protein; it acts as a negative regulator of CRK function by stabilizing a structure that inhibits the access by target proteins to the N-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes by intramolecular interactions, changing the subcellular localization of signal pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212693 [Multi-domain]  Cd Length: 57  Bit Score: 39.78  E-value: 3.13e-04
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gi 1622892340 1092 DVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11759     16 DKTALALEVGDLVKVTKINVSGQWEGELNGKVGHFPFTHVE 56
SH3_Vinexin_1 cd11921
First Src Homology 3 domain of Vinexin, also called Sorbin and SH3 domain containing 3 (Sorbs3) ...
1083-1134 3.15e-04

First Src Homology 3 domain of Vinexin, also called Sorbin and SH3 domain containing 3 (Sorbs3); Vinexin is also called Sorbs3, SH3P3, and SH3-containing adapter molecule 1 (SCAM-1). It is an adaptor protein containing one sorbin homology (SoHo) and three SH3 domains. Vinexin was first identified as a vinculin binding protein; it is co-localized with vinculin at cell-ECM and cell-cell adhesion sites. There are several splice variants of vinexin: alpha, which contains the SoHo and three SH3 domains and displays tissue-specific expression; and beta, which contains only the three SH3 domains and is widely expressed. Vinexin alpha stimulates the accumulation of F-actin at focal contact sites. Vinexin also promotes keratinocyte migration and wound healing. The SH3 domains of vinexin have been reported to bind a number of ligands including vinculin, WAVE2, DLG5, Abl, and Cbl. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212854  Cd Length: 55  Bit Score: 39.91  E-value: 3.15e-04
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEKI 1134
Cdd:cd11921      4 RLKFDFQAQSPKELTLQKGDIVYIHKEVDKNWLEGEHHGRVGIFPANYVEVL 55
SH3_CD2AP_1 cd12053
First Src Homology 3 domain (SH3A) of CD2-associated protein; CD2AP, also called CMS (Cas ...
1086-1134 3.23e-04

First Src Homology 3 domain (SH3A) of CD2-associated protein; CD2AP, also called CMS (Cas ligand with Multiple SH3 domains) or METS1 (Mesenchyme-to-Epithelium Transition protein with SH3 domains), is a cytosolic adaptor protein that plays a role in regulating the cytoskeleton. It is critical in cell-to-cell union necessary for kidney function. It also stabilizes the contact between a T cell and antigen-presenting cells. It is primarily expressed in podocytes at the cytoplasmic face of the slit diaphragm and serves as a linker anchoring podocin and nephrin to the actin cytoskeleton. CD2AP contains three SH3 domains, a proline-rich region, and a C-terminal coiled-coil domain. All of these domains enable CD2AP to bind various protein partners and assemble complexes that have been implicated in many different functions. This alignment model represents the first SH3 domain (SH3A) of CD2AP. SH3A binds to the PXXXPR motif present in c-Cbl and the cytoplasmic domain of cell adhesion protein CD2. Its interaction with CD2 anchors CD2 at sites of cell contact. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212986  Cd Length: 56  Bit Score: 39.83  E-value: 3.23e-04
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gi 1622892340 1086 YQYVGQDVDELSFNVNEVIEILME-DSSGWWKGRLHGQEGLFPGNYVEKI 1134
Cdd:cd12053      6 YDYDAVHEDELTIRVGEIIRNVKKlEEEGWLEGELNGRRGMFPDNFVKEI 55
SH3_Sorbs2_3 cd11917
Third (or C-terminal) Src Homology 3 domain of Sorbin and SH3 domain containing 2 (Sorbs2), ...
1076-1134 3.37e-04

Third (or C-terminal) Src Homology 3 domain of Sorbin and SH3 domain containing 2 (Sorbs2), also called Arg-binding protein 2 (ArgBP2); Sorbs2 or ArgBP2 is an adaptor protein containing one sorbin homology (SoHo) and three SH3 domains. It regulates actin-dependent processes including cell adhesion, morphology, and migration. It is expressed in many tissues and is abundant in the heart. Like vinexin, it is found in focal adhesion where it interacts with vinculin and afadin. It also localizes in epithelial cell stress fibers and in cardiac muscle cell Z-discs. Sorbs2 has been implicated to play roles in the signaling of c-Arg, Akt, and Pyk2. Other interaction partners of Sorbs2 include c-Abl, flotillin, spectrin, dynamin 1/2, synaptojanin, PTP-PEST, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212850 [Multi-domain]  Cd Length: 61  Bit Score: 39.98  E-value: 3.37e-04
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gi 1622892340 1076 RTHGPRCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKG--RLHGQEGLFPGNYVEKI 1134
Cdd:cd11917      1 QGGGEPFQALYNYMPRNEDELELREGDVIDVMEKCDDGWFVGtsRRTKFFGTFPGNYVKRL 61
SH3_Sorbs1_1 cd11919
First Src Homology 3 domain of Sorbin and SH3 domain containing 1 (Sorbs1), also called ponsin; ...
1083-1134 3.70e-04

First Src Homology 3 domain of Sorbin and SH3 domain containing 1 (Sorbs1), also called ponsin; Sorbs1 is also called ponsin, SH3P12, or CAP (c-Cbl associated protein). It is an adaptor protein containing one sorbin homology (SoHo) and three SH3 domains. It binds Cbl and plays a major role in regulating the insulin signaling pathway by enhancing insulin-induced phosphorylation of Cbl. Sorbs1, like vinexin, localizes at cell-ECM and cell-cell adhesion sites where it binds vinculin, paxillin, and afadin. It may function in the control of cell motility. Other interaction partners of Sorbs1 include c-Abl, Sos, flotillin, Grb4, ataxin-7, filamin C, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212852 [Multi-domain]  Cd Length: 55  Bit Score: 39.56  E-value: 3.70e-04
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gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEKI 1134
Cdd:cd11919      4 RAKFDFKAQTLKELPLQKGDIVYIYKQIDQNWYEGEHHGRVGIFPRSYIELL 55
SH3_Tec_like cd11768
Src Homology 3 domain of Tec-like Protein Tyrosine Kinases; The Tec (Tyrosine kinase expressed ...
1084-1133 3.75e-04

Src Homology 3 domain of Tec-like Protein Tyrosine Kinases; The Tec (Tyrosine kinase expressed in hepatocellular carcinoma) subfamily is composed of Tec, Btk, Bmx (Etk), Itk (Tsk, Emt), Rlk (Txk), and similar proteins. They are cytoplasmic (or nonreceptor) tyr kinases containing Src homology protein interaction domains (SH3, SH2) N-terminal to the catalytic tyr kinase domain. Most Tec subfamily members (except Rlk) also contain an N-terminal pleckstrin homology (PH) domain, which binds the products of PI3K and allows membrane recruitment and activation. In addition, some members contain the Tec homology (TH) domain, which contains proline-rich and zinc-binding regions. Tec kinases are expressed mainly by haematopoietic cells, although Tec and Bmx are also found in endothelial cells. B-cells express Btk and Tec, while T-cells express Itk, Txk, and Tec. Collectively, Tec kinases are expressed in a variety of myeloid cells such as mast cells, platelets, macrophages, and dendritic cells. Each Tec kinase shows a distinct cell-type pattern of expression. The function of Tec kinases in lymphoid cells have been studied extensively. They play important roles in the development, differentiation, maturation, regulation, survival, and function of B-cells and T-cells. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212702 [Multi-domain]  Cd Length: 54  Bit Score: 39.56  E-value: 3.75e-04
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGR-LHGQEGLFPGNYVEK 1133
Cdd:cd11768      4 ALYDFQPIEPGDLPLEKGEEYVVLDDSNEHWWRARdKNGNEGYIPSNYVTE 54
SH3_Shank cd11832
Src homology 3 domain of SH3 and multiple ankyrin repeat domains (Shank) proteins; Shank ...
1084-1127 4.53e-04

Src homology 3 domain of SH3 and multiple ankyrin repeat domains (Shank) proteins; Shank proteins carry scaffolding functions through multiple sites of protein-protein interaction in its domain architecture, including ankyrin (ANK) repeats, a long proline rich region, as well as SH3, PDZ, and SAM domains. They bind a variety of membrane and cytosolic proteins, and exist in alternatively spliced isoforms. They are highly enriched in postsynaptic density (PSD) where they interact with the cytoskeleton and with postsynaptic membrane receptors including NMDA and glutamate receptors. They are crucial in the construction and organization of the PSD and dendritic spines of excitatory synapses. There are three members of this family (Shank1, Shank2, Shank3) which show distinct and cell-type specific patterns of expression. Shank1 is brain-specific; Shank2 is found in neurons, glia, endocrine cells, liver, and kidney; Shank3 is widely expressed. The SH3 domain of Shank binds GRIP, a scaffold protein that binds AMPA receptors and Eph receptors/ligands. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212766  Cd Length: 50  Bit Score: 38.96  E-value: 4.53e-04
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFP 1127
Cdd:cd11832      4 AVKSYSPQEEGEISLHKGDRVKVLSIGEGGFWEGSVRGRTGWFP 47
SH3_ARHGEF9 cd11975
Src homology 3 domain of the Rho guanine nucleotide exchange factor ARHGEF9; ARHGEF9, also ...
1084-1131 4.59e-04

Src homology 3 domain of the Rho guanine nucleotide exchange factor ARHGEF9; ARHGEF9, also called PEM2 or collybistin, selectively activates Cdc42 by exchanging bound GDP for free GTP. It is highly expressed in the brain and it interacts with gephyrin, a postsynaptic protein associated with GABA and glycine receptors. Mutations in the ARHGEF9 gene cause X-linked mental retardation with associated features like seizures, hyper-anxiety, aggressive behavior, and sensory hyperarousal. ARHGEF9 contains a SH3 domain followed by RhoGEF (also called Dbl-homologous or DH) and Pleckstrin Homology (PH) domains. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212908  Cd Length: 62  Bit Score: 39.69  E-value: 4.59e-04
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYV 1131
Cdd:cd11975      9 AVWDHVTMANRELAFKAGDVIKVLDASNKDWWWGQIDDEEGWFPASFV 56
SH3_ASAP1 cd11965
Src homology 3 domain of ArfGAP with SH3 domain, ankyrin repeat and PH domain containing ...
1081-1131 5.02e-04

Src homology 3 domain of ArfGAP with SH3 domain, ankyrin repeat and PH domain containing protein 1; ASAP1 is also called DDEF1 (Development and Differentiation Enhancing Factor 1), AMAP1, centaurin beta-4, or PAG2. an Arf GTPase activating protein (GAP) with activity towards Arf1 and Arf5 but not Arf6. However, it has been shown to bind GTP-Arf6 stably without GAP activity. It has been implicated in cell growth, migration, and survival, as well as in tumor invasion and malignancy. It binds paxillin and cortactin, two components of invadopodia which are essential for tumor invasiveness. It also binds focal adhesion kinase (FAK) and the SH2/SH3 adaptor CrkL. ASAP1 contains an N-terminal BAR domain, followed by a Pleckstrin homology (PH) domain, an Arf GAP domain, ankyrin (ANK) repeats, and a C-terminal SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212898 [Multi-domain]  Cd Length: 57  Bit Score: 39.22  E-value: 5.02e-04
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gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQ---EGLFPGNYV 1131
Cdd:cd11965      1 RVKTIYDCQADNDDELTFVEGEVIIVTGEEDQEWWIGHIEGQperKGVFPVSFV 54
SH3_SH3RF_2 cd11787
Second Src Homology 3 domain of SH3 domain containing ring finger proteins; This model ...
1082-1130 5.24e-04

Second Src Homology 3 domain of SH3 domain containing ring finger proteins; This model represents the second SH3 domain of SH3RF1 (or POSH), SH3RF2 (or POSHER), SH3RF3 (POSH2), and similar domains. Members of this family are scaffold proteins that function as E3 ubiquitin-protein ligases. They all contain an N-terminal RING finger domain and multiple SH3 domains; SH3RF1 and SH3RF3 have four SH3 domains while SH3RF2 has three. SH3RF1 plays a role in calcium homeostasis through the control of the ubiquitin domain protein Herp. It may also have a role in regulating death receptor mediated and JNK mediated apoptosis. SH3RF3 interacts with p21-activated kinase 2 (PAK2) and GTP-loaded Rac1. It may play a role in regulating JNK mediated apoptosis in certain conditions. SH3RF2 acts as an anti-apoptotic regulator of the JNK pathway by binding to and promoting the degradation of SH3RF1. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212721 [Multi-domain]  Cd Length: 53  Bit Score: 38.85  E-value: 5.24e-04
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gi 1622892340 1082 CRALYQYVGQDVDE---LSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNY 1130
Cdd:cd11787      2 CKALYDFEMKDEDEkdcLTFKKGDVITVIRRVDENWAEGRLGDKIGIFPISF 53
SH3_NoxO1_2 cd12024
Second or C-terminal Src homology 3 domain of NADPH oxidase (Nox) Organizing protein 1; Nox ...
1088-1130 5.39e-04

Second or C-terminal Src homology 3 domain of NADPH oxidase (Nox) Organizing protein 1; Nox Organizing protein 1 (NoxO1) is a critical regulator of enzyme kinetics of the nonphagocytic NADPH oxidase Nox1, which catalyzes the transfer of electrons from NADPH to molecular oxygen to form superoxide. Nox1 is expressed in colon, stomach, uterus, prostate, and vascular smooth muscle cells. NoxO1 is involved in targeting activator subunits (such as NoxA1) to Nox1. It is co-localized with Nox1 in the membranes of resting cells and directs the subcellular localization of Nox1. NoxO1 contains an N-terminal Phox homology (PX) domain, tandem SH3 domains (N-SH3 and C-SH3), and a C-terminal proline-rich region (PRR). This model characterizes the second SH3 domain (or C-SH3) of NoxO1. The tandem SH3 domains of NoxO1 interact with the PRR of p22phox, which also complexes with Nox1. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212957  Cd Length: 53  Bit Score: 38.86  E-value: 5.39e-04
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gi 1622892340 1088 YVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNY 1130
Cdd:cd12024      8 YEAQKEDELSVPAGVVVEVLQKSDNGWWLIRYNGRAGYVPSMY 50
SH3_SH3RF1_3 cd11926
Third Src Homology 3 domain of SH3 domain containing ring finger 1, an E3 ubiquitin-protein ...
1084-1131 5.90e-04

Third Src Homology 3 domain of SH3 domain containing ring finger 1, an E3 ubiquitin-protein ligase; SH3RF1 is also called POSH (Plenty of SH3s) or SH3MD2 (SH3 multiple domains protein 2). It is a scaffold protein that acts as an E3 ubiquitin-protein ligase. It plays a role in calcium homeostasis through the control of the ubiquitin domain protein Herp. It may also have a role in regulating death receptor mediated and JNK mediated apoptosis. SH3RF1 also enhances the ubiquitination of ROMK1 potassium channel resulting in its increased endocytosis. It contains an N-terminal RING finger domain and four SH3 domains. This model represents the third SH3 domain, located in the middle, of SH3RF1. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212859 [Multi-domain]  Cd Length: 55  Bit Score: 38.80  E-value: 5.90e-04
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKG-RLH-GQEGLFPGNYV 1131
Cdd:cd11926      4 AIYPYTPRKEDELELRKGEMFLVFERCQDGWFKGtSMHtSKIGVFPGNYV 53
Herpes_LP pfam03363
Herpesvirus leader protein;
952-1081 1.07e-03

Herpesvirus leader protein;


Pssm-ID: 281372 [Multi-domain]  Cd Length: 174  Bit Score: 41.24  E-value: 1.07e-03
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gi 1622892340  952 KSSKPTRKGMAKGRPRRSSQAPTRAAPTRAAPGPPRGmDRNGVPPSARGGPLPLEimsggsshrpPRGPPSTSLgasRRP 1031
Cdd:pfam03363   32 RSPSPTRGGQEPRRVRRRVLVQQEEEVVSGSPSGPRG-DRSEGPGPARPGPPGIG----------PEGPLGQLL---RRH 97
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gi 1622892340 1032 RAQLPSEHNTEFLNVPDQGMagMQRKRSVGQRPVPGVGRPKPQPRTHGPR 1081
Cdd:pfam03363   98 RSPSPTRGGQEPRRVRRRVL--VQQEEEVVSGSPSGPLRPRPQPPAQSLR 145
SH3_DOCK_AB cd11872
Src Homology 3 domain of Class A and B Dedicator of Cytokinesis proteins; DOCK proteins are ...
1084-1131 1.13e-03

Src Homology 3 domain of Class A and B Dedicator of Cytokinesis proteins; DOCK proteins are atypical guanine nucleotide exchange factors (GEFs) that lack the conventional Dbl homology (DH) domain. They are divided into four classes (A-D) based on sequence similarity and domain architecture: class A includes Dock1, 2 and 5; class B includes Dock3 and 4; class C includes Dock6, 7, and 8; and class D includes Dock9, 10 and 11. All DOCKs contain two homology domains: the DHR-1 (Dock homology region-1), also called CZH1 (CED-5, Dock180, and MBC-zizimin homology 1), and DHR-2 (also called CZH2 or Docker). The DHR-1 domain binds phosphatidylinositol-3,4,5-triphosphate while DHR-2 contains the catalytic activity for Rac and/or Cdc42. This subfamily includes only Class A and B DOCKs, which also contain an SH3 domain at the N-terminal region and a PxxP motif at the C-terminus. Class A/B DOCKs are mostly specific GEFs for Rac, except Dock4 which activates the Ras family GTPase Rap1, probably indirectly through interaction with Rap regulatory proteins. The SH3 domain of class A/B DOCKs have been shown to bind Elmo, a scaffold protein that promotes GEF activity of DOCKs by releasing DHR-2 autoinhibition by the intramolecular SH3 domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212805 [Multi-domain]  Cd Length: 56  Bit Score: 37.95  E-value: 1.13e-03
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILmEDSSGWWKG---RLHGQEGLFPGNYV 1131
Cdd:cd11872      4 AIYNFQGDGEHQLSLQVGDTVQIL-EECEGWYRGfslRNKSLKGIFPKSYV 53
SH3_Intersectin2_4 cd11994
Fourth Src homology 3 domain (or SH3D) of Intersectin-2; Intersectin-2 (ITSN2) is an adaptor ...
1088-1132 1.18e-03

Fourth Src homology 3 domain (or SH3D) of Intersectin-2; Intersectin-2 (ITSN2) is an adaptor protein that functions in exo- and endocytosis, actin cytoskeletal reorganization, and signal transduction. It plays a role in clathrin-coated pit (CCP) formation. It binds to many proteins through its multidomain structure and facilitate the assembly of multimeric complexes. ITSN2 also functions as a specific GEF for Cdc42 activation in epithelial morphogenesis, and is required in mitotic spindle orientation. It exists in alternatively spliced short and long isoforms. The short isoform contains two Eps15 homology domains (EH1 and EH2), a coiled-coil region and five SH3 domains (SH3A-E), while the long isoform, in addition, contains RhoGEF (also called Dbl-homologous or DH), Pleckstrin homology (PH) and C2 domains. The fourth SH3 domain (or SH3D) of ITSN2 is expected to bind protein partners, similar to ITSN1 which has been shown to bind SHIP2, Numb, CdGAP, and N-WASP. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212927  Cd Length: 59  Bit Score: 38.37  E-value: 1.18e-03
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gi 1622892340 1088 YVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHG-----QEGLFPGNYVE 1132
Cdd:cd11994      8 YVASGVEQLSLSPGQLILILKKNSSGWWLGELQArgkkrQKGWFPASHVK 57
SH3_DNMBP_C2_like cd11800
Second C-terminal Src homology 3 domain of Dynamin Binding Protein, also called Tuba, and ...
1084-1133 1.18e-03

Second C-terminal Src homology 3 domain of Dynamin Binding Protein, also called Tuba, and similar domains; DNMBP or Tuba is a cdc42-specific guanine nucleotide exchange factor (GEF) that contains four N-terminal SH3 domains, a central RhoGEF [or Dbl homology (DH)] domain followed by a Bin/Amphiphysin/Rvs (BAR) domain, and two C-terminal SH3 domains. It provides a functional link between dynamin, Rho GTPase signaling, and actin dynamics. It plays an important role in regulating cell junction configuration. The C-terminal SH3 domains of DNMBP bind to N-WASP and Ena/VASP proteins, which are key regulatory proteins of the actin cytoskeleton. Also included in this subfamily is the second C-terminal SH3 domain of Rho guanine nucleotide exchange factor 37 (ARHGEF37), whose function is still unknown. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212734 [Multi-domain]  Cd Length: 57  Bit Score: 38.12  E-value: 1.18e-03
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEIL-MEDSSG---WWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11800      4 ALYTFEARSPGELSVTEGQVVTVLeKHDLKGnpeWWLVEDRGKQGYVPSNYLAK 57
SH3_DNMBP_N4 cd11797
Fourth N-terminal Src homology 3 domain of Dynamin Binding Protein, also called Tuba; DNMBP or ...
1084-1127 1.40e-03

Fourth N-terminal Src homology 3 domain of Dynamin Binding Protein, also called Tuba; DNMBP or Tuba is a cdc42-specific guanine nucleotide exchange factor (GEF) that contains four N-terminal SH3 domains, a central RhoGEF [or Dbl homology (DH)] domain followed by a Bin/Amphiphysin/Rvs (BAR) domain, and two C-terminal SH3 domains. It provides a functional link between dynamin and key regulatory proteins of the actin cytoskeleton. It plays an important role in regulating cell junction configuration. The four N-terminal SH3 domains of DNMBP bind the GTPase dynamin, which plays an important role in the fission of endocytic vesicles. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212731  Cd Length: 50  Bit Score: 37.79  E-value: 1.40e-03
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFP 1127
Cdd:cd11797      4 ALYRFQALEPNELDFEVGDRIRIIATLEDGWLEGELKGRRGIFP 47
SH3_Lck cd12005
Src homology 3 domain of Lck Protein Tyrosine Kinase; Lck is a member of the Src subfamily of ...
1084-1133 1.54e-03

Src homology 3 domain of Lck Protein Tyrosine Kinase; Lck is a member of the Src subfamily of proteins, which are cytoplasmic (or non-receptor) PTKs. Lck is expressed in T-cells and natural killer cells. It plays a critical role in T-cell maturation, activation, and T-cell receptor (TCR) signaling. Lck phosphorylates ITAM (immunoreceptor tyr activation motif) sequences on several subunits of TCRs, leading to the activation of different second messenger cascades. Phosphorylated ITAMs serve as binding sites for other signaling factor such as Syk and ZAP-70, leading to their activation and propagation of downstream events. In addition, Lck regulates drug-induced apoptosis by interfering with the mitochondrial death pathway. The apototic role of Lck is independent of its primary function in T-cell signaling. Src kinases contain an N-terminal SH4 domain with a myristoylation site, followed by SH3 and SH2 domains, a tyr kinase domain, and a regulatory C-terminal region containing a conserved tyr. They are activated by autophosphorylation at the tyr kinase domain, but are negatively regulated by phosphorylation at the C-terminal tyr by Csk (C-terminal Src Kinase). The SH3 domain of Src kinases contributes to substrate recruitment by binding adaptor proteins/substrates, and regulation of kinase activity through an intramolecular interaction. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212938 [Multi-domain]  Cd Length: 54  Bit Score: 37.88  E-value: 1.54e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|..
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSgWWKGR--LHGQEGLFPGNYVEK 1133
Cdd:cd12005      4 ALYSYEPSHDGDLGFEKGEKLRILEQSGE-WWKAQslTTGQEGFIPFNFVAK 54
SH3_Alpha_Spectrin cd11808
Src homology 3 domain of Alpha Spectrin; Spectrin is a major structural component of the red ...
1084-1133 1.67e-03

Src homology 3 domain of Alpha Spectrin; Spectrin is a major structural component of the red blood cell membrane skeleton and is important in erythropoiesis and membrane biogenesis. It is a flexible, rope-like molecule composed of two subunits, alpha and beta, which consist of many spectrin-type repeats. Alpha and beta spectrin associate to form heterodimers and tetramers; spectrin tetramer formation is critical for red cell shape and deformability. Defects in alpha spectrin have been associated with inherited hemolytic anemias including hereditary spherocytosis (HSp), hereditary elliptocytosis (HE), and hereditary pyropoikilocytosis (HPP). Alpha spectrin contains a middle SH3 domain and a C-terminal EF-hand binding motif in addition to multiple spectrin repeats. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212742 [Multi-domain]  Cd Length: 53  Bit Score: 37.46  E-value: 1.67e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd11808      4 ALYDYQEKSPREVSMKKGDILTLLNSSNKDWWKVEVNDRQGFVPAAYVKK 53
SH3_SPIN90 cd11849
Src homology 3 domain of SH3 protein interacting with Nck, 90 kDa (SPIN90); SPIN90 is also ...
1083-1132 1.99e-03

Src homology 3 domain of SH3 protein interacting with Nck, 90 kDa (SPIN90); SPIN90 is also called NCK interacting protein with SH3 domain (NCKIPSD), Dia-interacting protein (DIP), 54 kDa vimentin-interacting protein (VIP54), or WASP-interacting SH3-domain protein (WISH). It is an F-actin binding protein that regulates actin polymerization and endocytosis. It associates with the Arp2/3 complex near actin filaments and determines filament localization at the leading edge of lamellipodia. SPIN90 is expressed in the early stages of neuronal differentiation and plays a role in regulating growth cone dynamics and neurite outgrowth. It also interacts with IRSp53 and regulates cell motility by playing a role in the formation of membrane protrusions. SPIN90 contains an N-terminal SH3 domain, a proline-rich domain, and a C-terminal VCA (verprolin-homology and cofilin-like acidic) domain. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212783 [Multi-domain]  Cd Length: 53  Bit Score: 37.29  E-value: 1.99e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSSGWWK-GRLHGQEGLFPGNYVE 1132
Cdd:cd11849      3 RALYDFKSAEPNTLSFSEGETFLLLERSNAHWWLvTNHSGETGYVPANYVK 53
SH3_Tks5_4 cd12019
Fourth Src homology 3 domain of Tyrosine kinase substrate with five SH3 domains; Tks5, also ...
1086-1132 2.02e-03

Fourth Src homology 3 domain of Tyrosine kinase substrate with five SH3 domains; Tks5, also called SH3 and PX domain-containing protein 2A (SH3PXD2A) or Five SH (FISH), is a scaffolding protein and Src substrate that is localized in podosomes, which are electron-dense structures found in Src-transformed fibroblasts, osteoclasts, macrophages, and some invasive cancer cells. It binds and regulates some members of the ADAMs family of transmembrane metalloproteases, which function as sheddases and mediators of cell and matrix interactions. It is required for podosome formation, degradation of the extracellular matrix, and cancer cell invasion. Tks5 contains an N-terminal Phox homology (PX) domain and five SH3 domains. This model characterizes the fourth SH3 domain of Tks5. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212952  Cd Length: 53  Bit Score: 37.27  E-value: 2.02e-03
                           10        20        30        40
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gi 1622892340 1086 YQYVgQDvDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd12019      8 YQKV-QD-SEISFPAGVEVEVLEKQESGWWYVRFGELEGWAPSHYLE 52
SH3_DOCK1_5_A cd12051
Src Homology 3 domain of Class A Dedicator of Cytokinesis proteins 1 and 5; Dock1, also called ...
1084-1131 2.52e-03

Src Homology 3 domain of Class A Dedicator of Cytokinesis proteins 1 and 5; Dock1, also called Dock180, and Dock5 are class A DOCKs and are atypical guanine nucleotide exchange factors (GEFs) that lack the conventional Dbl homology (DH) domain. Dock1 interacts with the scaffold protein Elmo and the resulting complex functions upstream of Rac in many biological events including phagocytosis of apoptotic cells, cell migration and invasion. Dock5 functions upstream of Rac1 to regulate osteoclast function. All DOCKs contain two homology domains: the DHR-1 (Dock homology region-1), also called CZH1 (CED-5, Dock180, and MBC-zizimin homology 1), and DHR-2 (also called CZH2 or Docker). The DHR-1 domain binds phosphatidylinositol-3,4,5-triphosphate while DHR-2 contains the catalytic activity for Rac and/or Cdc42. Class A DOCKs also contain an SH3 domain at the N-terminal region and a PxxP motif at the C-terminus; they are specific GEFs for Rac. The SH3 domain of Dock1 binds to DHR-2 in an autoinhibitory manner; binding of Elmo to the SH3 domain of Dock1 exposes the DHR-2 domain and promotes GEF activity. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212984 [Multi-domain]  Cd Length: 56  Bit Score: 37.11  E-value: 2.52e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILmEDSSGWWKG---RLHGQEGLFPGNYV 1131
Cdd:cd12051      4 AIYNYDARGPDELSLQIGDTVHIL-ETYEGWYRGytlRKKSKKGIFPASYI 53
ABC_NikE_OppD_transporters cd03257
ATP-binding cassette domain of nickel/oligopeptides specific transporters; The ABC transporter ...
102-132 2.72e-03

ATP-binding cassette domain of nickel/oligopeptides specific transporters; The ABC transporter subfamily specific for the transport of dipeptides, oligopeptides (OppD), and nickel (NikDE). The NikABCDE system of E. coli belongs to this family and is composed of the periplasmic binding protein NikA, two integral membrane components (NikB and NikC), and two ATPase (NikD and NikE). The NikABCDE transporter is synthesized under anaerobic conditions to meet the increased demand for nickel resulting from hydrogenase synthesis. The molecular mechanism of nickel uptake in many bacteria and most archaea is not known. Many other members of this ABC family are also involved in the uptake of dipeptides and oligopeptides. The oligopeptide transport system (Opp) is a five-component ABC transport composed of a membrane-anchored substrate binding proteins (SRP), OppA, two transmembrane proteins, OppB and OppC, and two ATP-binding domains, OppD and OppF.


Pssm-ID: 213224 [Multi-domain]  Cd Length: 228  Bit Score: 40.57  E-value: 2.72e-03
                           10        20        30
                   ....*....|....*....|....*....|.
gi 1622892340  102 ENQCVIISGESGAGKTVAAKYIMGYISKVSG 132
Cdd:cd03257     30 KGETLGLVGESGSGKSTLARAILGLLKPTSG 60
SH3_SKAP1 cd12044
Src Homology 3 domain of Src Kinase-Associated Phosphoprotein 1; SKAP1, also called SKAP55 ...
1083-1131 2.85e-03

Src Homology 3 domain of Src Kinase-Associated Phosphoprotein 1; SKAP1, also called SKAP55 (Src kinase-associated protein of 55kDa), is an immune cell-specific adaptor protein that plays an important role in T-cell adhesion, migration, and integrin clustering. It is expressed exclusively in T-lymphocytes, mast cells, and macrophages. Binding partners include ADAP (adhesion and degranulation-promoting adaptor protein), Fyn, Riam, RapL, and RasGRP. It contains a pleckstrin homology (PH) domain, a C-terminal SH3 domain, and several tyrosine phosphorylation sites. The SH3 domain of SKAP1 is necessary for its ability to regulate T-cell conjugation with antigen-presenting cells and the formation of LFA-1 clusters. SKAP1 binds primarily to a proline-rich region of ADAP through its SH3 domain; its degradation is regulated by ADAP. A secondary interaction occurs via the ADAP SH3 domain and the RKxxYxxY motif in SKAP1. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212977  Cd Length: 53  Bit Score: 37.15  E-value: 2.85e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1083 RALYQYVGQDVDELSFNVNEVIEILMEDSS--GWWKGRLHGQEGLFPGNYV 1131
Cdd:cd12044      3 QGLWDCFGDNPDELSFQRGDLIYILSKEYNmyGWWVGELNGIVGIVPKDYL 53
SH3_Irsp53_BAIAP2L cd11779
Src Homology 3 domain of Insulin Receptor tyrosine kinase Substrate p53, Brain-specific ...
1080-1133 2.91e-03

Src Homology 3 domain of Insulin Receptor tyrosine kinase Substrate p53, Brain-specific Angiogenesis Inhibitor 1-Associated Protein 2 (BAIAP2)-Like proteins, and similar proteins; Proteins in this family include IRSp53, BAIAP2L1, BAIAP2L2, and similar proteins. They all contain an Inverse-Bin/Amphiphysin/Rvs (I-BAR) or IMD domain in addition to the SH3 domain. IRSp53, also known as BAIAP2, is a scaffolding protein that takes part in many signaling pathways including Cdc42-induced filopodia formation, Rac-mediated lamellipodia extension, and spine morphogenesis. IRSp53 exists as multiple splicing variants that differ mainly at the C-termini. BAIAP2L1, also called IRTKS (Insulin Receptor Tyrosine Kinase Substrate), serves as a substrate for the insulin receptor and binds the small GTPase Rac. It plays a role in regulating the actin cytoskeleton and colocalizes with F-actin, cortactin, VASP, and vinculin. IRSp53 and IRTKS also mediate the recruitment of effector proteins Tir and EspFu, which regulate host cell actin reorganization, to bacterial attachment sites. BAIAP2L2 co-localizes with clathrin plaques but its function has not been determined. The SH3 domains of IRSp53 and IRTKS have been shown to bind the proline-rich C-terminus of EspFu. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212713 [Multi-domain]  Cd Length: 57  Bit Score: 36.92  E-value: 2.91e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*..
gi 1622892340 1080 PRCRALYQYVGQDVDELSFNVNEVIEILM-EDSSGWWKGRLH--GQEGLFPGNYVEK 1133
Cdd:cd11779      1 PRVKALYPHAAGGETQLSFEEGDVITLLGpEPRDGWHYGENErsGRRGWFPIAYTEP 57
SH3_p67phox-like_C cd11870
C-terminal Src Homology 3 domain of the p67phox subunit of NADPH oxidase and similar proteins; ...
1084-1132 3.01e-03

C-terminal Src Homology 3 domain of the p67phox subunit of NADPH oxidase and similar proteins; This subfamily is composed of p67phox, NADPH oxidase activator 1 (Noxa1), and similar proteins. p67phox, also called Neutrophil cytosol factor 2 (NCF-2), and Noxa1 are homologs and are the cytosolic subunits of the phagocytic (Nox2) and nonphagocytic (Nox1) NADPH oxidase complexes, respectively. NADPH oxidase catalyzes the transfer of electrons from NADPH to oxygen during phagocytosis forming superoxide and reactive oxygen species. p67phox and Noxa1 play regulatory roles. p67phox contains N-terminal TPR, first SH3 (or N-terminal or central SH3), PB1, and C-terminal SH3 domains. Noxa1 has a similar domain architecture except it is lacking the N-terminal SH3 domain. The TPR domain of both binds activated GTP-bound Rac, while the C-terminal SH3 domain of p67phox and Noxa1 binds the polyproline motif found at the C-terminus of p47phox and Noxo1, respectively. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212803 [Multi-domain]  Cd Length: 53  Bit Score: 36.74  E-value: 3.01e-03
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*....
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVE 1132
Cdd:cd11870      4 ALHRYEAQGPEDLGFREGDTIDVLSEVNEAWLEGHSDGRVGIFPKCFVV 52
PRK07764 PRK07764
DNA polymerase III subunits gamma and tau; Validated
956-1080 3.56e-03

DNA polymerase III subunits gamma and tau; Validated


Pssm-ID: 236090 [Multi-domain]  Cd Length: 824  Bit Score: 41.51  E-value: 3.56e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  956 PTRKGMAKGRPRRSSQAPTRAAPTRAAPGPPRGMDrnGVPPSARGGPLPLEIMSGGSSHRPPRGPPSTSLGASRrPRAQL 1035
Cdd:PRK07764   633 AAAPAEASAAPAPGVAAPEHHPKHVAVPDASDGGD--GWPAKAGGAAPAAPPPAPAPAAPAAPAGAAPAQPAPA-PAATP 709
                           90       100       110       120
                   ....*....|....*....|....*....|....*....|....*
gi 1622892340 1036 PSEHNTEFLNVPDQGMAGMQRKRSVGQRPVPGVGRPKPQPRTHGP 1080
Cdd:PRK07764   710 PAGQADDPAAQPPQAAQGASAPSPAADDPVPLPPEPDDPPDPAGA 754
SH3_Tec cd11905
Src Homology 3 domain of Tec (Tyrosine kinase expressed in hepatocellular carcinoma); Tec is a ...
1084-1131 3.60e-03

Src Homology 3 domain of Tec (Tyrosine kinase expressed in hepatocellular carcinoma); Tec is a cytoplasmic (or nonreceptor) tyr kinase containing Src homology protein interaction domains (SH3, SH2) N-terminal to the catalytic tyr kinase domain. It also contains an N-terminal pleckstrin homology (PH) domain, which binds the products of PI3K and allows membrane recruitment and activation, and the Tec homology (TH) domain, which contains proline-rich and zinc-binding regions. It is more widely-expressed than other Tec subfamily kinases. Tec is found in endothelial cells, both B- and T-cells, and a variety of myeloid cells including mast cells, erythroid cells, platelets, macrophages and neutrophils. Tec is a key component of T-cell receptor (TCR) signaling, and is important in TCR-stimulated proliferation, IL-2 production and phospholipase C-gamma1 activation. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212838 [Multi-domain]  Cd Length: 56  Bit Score: 36.72  E-value: 3.60e-03
                           10        20        30        40
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGR-LHGQEGLFPGNYV 1131
Cdd:cd11905      5 AMYDFQPTEPHDLRLETGEEYVILEKNDVHWWKARdKYGKEGYIPSNYV 53
SH3_Sorbs1_2 cd11922
Second Src Homology 3 domain of Sorbin and SH3 domain containing 1 (Sorbs1), also called ...
1084-1134 4.24e-03

Second Src Homology 3 domain of Sorbin and SH3 domain containing 1 (Sorbs1), also called ponsin; Sorbs1 is also called ponsin, SH3P12, or CAP (c-Cbl associated protein). It is an adaptor protein containing one sorbin homology (SoHo) and three SH3 domains. It binds Cbl and plays a major role in regulating the insulin signaling pathway by enhancing insulin-induced phosphorylation of Cbl. Sorbs1, like vinexin, localizes at cell-ECM and cell-cell adhesion sites where it binds vinculin, paxillin, and afadin. It may function in the control of cell motility. Other interaction partners of Sorbs1 include c-Abl, Sos, flotillin, Grb4, ataxin-7, filamin C, among others. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212855 [Multi-domain]  Cd Length: 58  Bit Score: 36.51  E-value: 4.24e-03
                           10        20        30        40        50
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gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHG--QEGLFPGNYVEKI 1134
Cdd:cd11922      5 AKFNFNGDTQVEMSFRKGERITLLRQVDENWYEGRIPGtsRQGIFPITYVDVI 57
SH3_p47phox_2 cd12022
Second or C-terminal Src homology 3 domain of the p47phox subunit of NADPH oxidase, also ...
1088-1133 4.77e-03

Second or C-terminal Src homology 3 domain of the p47phox subunit of NADPH oxidase, also called Neutrophil Cytosolic Factor 1; p47phox, or NCF1, is a cytosolic subunit of the phagocytic NADPH oxidase complex (also called Nox2 or gp91phox), which plays a key role in the ability of phagocytes to defend against bacterial infections. NADPH oxidase catalyzes the transfer of electrons from NADPH to oxygen during phagocytosis forming superoxide and reactive oxygen species. p47phox is required for activation of NADH oxidase and plays a role in translocation. It contains an N-terminal Phox homology (PX) domain, tandem SH3 domains (N-SH3 and C-SH3), a polybasic/autoinhibitory region, and a C-terminal proline-rich region (PRR). This model characterizes the second SH3 domain (or C-SH3) of p47phox. In its inactive state, the tandem SH3 domains interact intramolecularly with the autoinhibitory region; upon activation, the tandem SH3 domains are exposed through a conformational change, resulting in their binding to the PRR of p22phox and the activation of NADPH oxidase. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212955 [Multi-domain]  Cd Length: 53  Bit Score: 36.36  E-value: 4.77e-03
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*.
gi 1622892340 1088 YVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHGQEGLFPGNYVEK 1133
Cdd:cd12022      8 YTAVEEDELTLLEGEAIEVIHKLLDGWWVVRKGEVTGYFPSMYLQK 53
SH3_Nck1_1 cd11900
First Src Homology 3 domain of Nck1 adaptor protein; Nck1 (also called Nckalpha) plays a ...
1084-1133 4.94e-03

First Src Homology 3 domain of Nck1 adaptor protein; Nck1 (also called Nckalpha) plays a crucial role in connecting signaling pathways of tyrosine kinase receptors and important effectors in actin dynamics and cytoskeletal remodeling. It binds and activates RasGAP, resulting in the downregulation of Ras. It is also involved in the signaling of endothilin-mediated inhibition of cell migration. Nck adaptor proteins regulate actin cytoskeleton dynamics by linking proline-rich effector molecules to protein tyrosine kinases and phosphorylated signaling intermediates. They contain three SH3 domains and a C-terminal SH2 domain. They function downstream of the PDGFbeta receptor and are involved in Rho GTPase signaling and actin dynamics. Vertebrates contain two Nck adaptor proteins: Nck1 (also called Nckalpha) and Nck2, which show partly overlapping functions but also bind distinct targets. The first SH3 domain of Nck1 binds the PxxDY sequence in the CD3e cytoplasmic tail; this binding inhibits phosphorylation by Src kinases, resulting in the downregulation of TCR surface expression. SH3 domains are protein interaction domains that usually bind to proline-rich ligands with moderate affinity and selectivity, preferentially a PxxP motif. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212833 [Multi-domain]  Cd Length: 59  Bit Score: 36.62  E-value: 4.94e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIeILMEDSSGWWKGR-LHGQEGLFPGNYVEK 1133
Cdd:cd11900      7 AKFDYVAQQDQELDIKKNERL-WLLDDSKSWWRVRnAMNKTGFVPSNYVER 56
SH3_Vinexin_2 cd11924
Second Src Homology 3 domain of Vinexin, also called Sorbin and SH3 domain containing 3 ...
1084-1132 4.96e-03

Second Src Homology 3 domain of Vinexin, also called Sorbin and SH3 domain containing 3 (Sorbs3); Vinexin is also called Sorbs3, SH3P3, and SH3-containing adapter molecule 1 (SCAM-1). It is an adaptor protein containing one sorbin homology (SoHo) and three SH3 domains. Vinexin was first identified as a vinculin binding protein; it is co-localized with vinculin at cell-ECM and cell-cell adhesion sites. There are several splice variants of vinexin: alpha, which contains the SoHo and three SH3 domains and displays tissue-specific expression; and beta, which contains only the three SH3 domains and is widely expressed. Vinexin alpha stimulates the accumulation of F-actin at focal contact sites. Vinexin also promotes keratinocyte migration and wound healing. The SH3 domains of vinexin have been reported to bind a number of ligands including vinculin, WAVE2, DLG5, Abl, and Cbl. SH3 domains are protein interaction domains that bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs. They play versatile and diverse roles in the cell including the regulation of enzymes, changing the subcellular localization of signaling pathway components, and mediating the formation of multiprotein complex assemblies.


Pssm-ID: 212857  Cd Length: 56  Bit Score: 36.48  E-value: 4.96e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1084 ALYQYVGQDVDELSFNVNEVIEILMEDSSGWWKGRLHG--QEGLFPGNYVE 1132
Cdd:cd11924      5 AQYTFKGDLEVELSFRKGEHICLIRKVNENWYEGRITGtgRQGIFPASYVQ 55
SH3_SH3TC cd11885
Src Homology 3 domain of SH3 domain and tetratricopeptide repeat-containing (SH3TC) proteins ...
1081-1131 5.65e-03

Src Homology 3 domain of SH3 domain and tetratricopeptide repeat-containing (SH3TC) proteins and similar domains; This subfamily is composed of vertebrate SH3TC proteins and hypothetical fungal proteins containing BAR and SH3 domains. Mammals contain two SH3TC proteins, SH3TC1 and SH3TC2. The function of SH3TC1 is unknown. SH3TC2 is localized in Schwann cells in the peripheral nervous system, where it interacts with Rab11 and plays a role in peripheral nerve myelination. Mutations in SH3TC2 are associated with Charcot-Marie-Tooth disease type 4C, a severe hereditary peripheral neuropathy with symptoms that include progressive scoliosis, delayed age of walking, muscular atrophy, distal weakness, and reduced nerve conduction velocity. SH3 domains bind to proline-rich ligands with moderate affinity and selectivity, preferentially to PxxP motifs; they play a role in the regulation of enzymes by intramolecular interactions, changing the subcellular localization of signal pathway components and mediate multiprotein complex assemblies.


Pssm-ID: 212818  Cd Length: 55  Bit Score: 36.14  E-value: 5.65e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*
gi 1622892340 1081 RCRALYQYVGQDVDELSFNVNEVIEILME--DSSGWWKGR--LHGQEGLFPGNYV 1131
Cdd:cd11885      1 SCTAKMDFEGVEPGELSFRQGDSIEIIGDliPGLQWFVGRskSSGRVGFVPTNHF 55
PRK07764 PRK07764
DNA polymerase III subunits gamma and tau; Validated
950-1080 5.92e-03

DNA polymerase III subunits gamma and tau; Validated


Pssm-ID: 236090 [Multi-domain]  Cd Length: 824  Bit Score: 40.74  E-value: 5.92e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1622892340  950 LPkSSKPTRKGMAKGRPRRSSQAPTRAAPTRAAPGPPRGMDRNGVPPSARGGPLPleimSGGSSHRPPRGPPSTSLGASR 1029
Cdd:PRK07764   364 LP-SASDDERGLLARLERLERRLGVAGGAGAPAAAAPSAAAAAPAAAPAPAAAAP----AAAAAPAPAAAPQPAPAPAPA 438
                           90       100       110       120       130
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1622892340 1030 RPRAQLPSEHNTEFLNVPDQGMAGMQRKRSVGQRPVPGVGRPKPQPRTHGP 1080
Cdd:PRK07764   439 PAPPSPAGNAPAGGAPSPPPAAAPSAQPAPAPAAAPEPTAAPAPAPPAAPA 489
Motor_domain cd01363
Myosin and Kinesin motor domain; Myosin and Kinesin motor domain. These ATPases belong to the ...
559-587 7.65e-03

Myosin and Kinesin motor domain; Myosin and Kinesin motor domain. These ATPases belong to the P-loop NTPase family and provide the driving force in myosin and kinesin mediated processes. Some of the names do not match with what is given in the sequence list. This is because they are based on the current nomenclature by Kollmar/Sebe-Pedros.


Pssm-ID: 276814 [Multi-domain]  Cd Length: 170  Bit Score: 38.48  E-value: 7.65e-03
                           10        20        30
                   ....*....|....*....|....*....|
gi 1622892340  559 AGS-KIKKQANDLVATLMRCTPHYIRCIKP 587
Cdd:cd01363    141 AGFeIINESLNTLMNVLRATRPHFVRCISP 170
 
Blast search parameters
Data Source: Precalculated data, version = cdd.v.3.21
Preset Options:Database: CDSEARCH/cdd   Low complexity filter: no  Composition Based Adjustment: yes   E-value threshold: 0.01

References:

  • Wang J et al. (2023), "The conserved domain database in 2023", Nucleic Acids Res.51(D)384-8.
  • Lu S et al. (2020), "The conserved domain database in 2020", Nucleic Acids Res.48(D)265-8.
  • Marchler-Bauer A et al. (2017), "CDD/SPARCLE: functional classification of proteins via subfamily domain architectures.", Nucleic Acids Res.45(D)200-3.
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