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Conserved domains on  [gi|1034596152|ref|XP_016879221|]
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3 beta-hydroxysteroid dehydrogenase type 7 isoform X2 [Homo sapiens]

Protein Classification

Rossmann-fold NAD(P)-binding domain-containing protein( domain architecture ID 229380)

Rossmann-fold NAD(P)-binding domain-containing protein may function as an oxidoreductase

Graphical summary

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List of domain hits

Name Accession Description Interval E-value
NADB_Rossmann super family cl21454
Rossmann-fold NAD(P)(+)-binding proteins; A large family of proteins that share a ...
11-177 1.15e-92

Rossmann-fold NAD(P)(+)-binding proteins; A large family of proteins that share a Rossmann-fold NAD(P)H/NAD(P)(+) binding (NADB) domain. The NADB domain is found in numerous dehydrogenases of metabolic pathways such as glycolysis, and many other redox enzymes. NAD binding involves numerous hydrogen-bonds and van der Waals contacts, in particular H-bonding of residues in a turn between the first strand and the subsequent helix of the Rossmann-fold topology. Characteristically, this turn exhibits a consensus binding pattern similar to GXGXXG, in which the first 2 glycines participate in NAD(P)-binding, and the third facilitates close packing of the helix to the beta-strand. Typically, proteins in this family contain a second domain in addition to the NADB domain, which is responsible for specifically binding a substrate and catalyzing a particular enzymatic reaction.


The actual alignment was detected with superfamily member cd09811:

Pssm-ID: 473865 [Multi-domain]  Cd Length: 354  Bit Score: 274.38  E-value: 1.15e-92
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  11 VYLVTGGCGFLGEHVVRMLLQREPRLGELRVFDQHLGPWLEELK---TGPVRVTAIQGDVTQAHEVAAAVAGAHVVIHTA 87
Cdd:cd09811     1 VCLVTGGGGFLGQHIIRLLLERKEELKEIRVLDKAFGPELIEHFeksQGKTYVTDIEGDIKDLSFLFRACQGVSVVIHTA 80
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  88 GLVDVFGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKGHPFYRGNEDTPYEAVHRHPYPCSKALAE 167
Cdd:cd09811    81 AIVDVFGPPNYEELEEVNVNGTQAVLEACVQNNVKRLVYTSSIEVAGPNFKGRPIFNGVEDTPYEDTSTPPYASSKLLAE 160
                         170
                  ....*....|
gi 1034596152 168 WLVLEANGRK 177
Cdd:cd09811   161 NIVLNANGAP 170
 
Name Accession Description Interval E-value
3b-HSD_HSDB1_like_SDR_e cd09811
human 3beta-HSD (hydroxysteroid dehydrogenase) and HSD3B1(delta 5-delta 4-isomerase)-like, ...
11-177 1.15e-92

human 3beta-HSD (hydroxysteroid dehydrogenase) and HSD3B1(delta 5-delta 4-isomerase)-like, extended (e) SDRs; This extended-SDR subgroup includes human 3 beta-HSD/HSD3B1 and C(27) 3beta-HSD/ [3beta-hydroxy-delta(5)-C(27)-steroid oxidoreductase; HSD3B7], and related proteins. These proteins have the characteristic active site tetrad and NAD(P)-binding motif of extended SDRs. 3 beta-HSD catalyzes the oxidative conversion of delta 5-3 beta-hydroxysteroids to the delta 4-3-keto configuration; this activity is essential for the biosynthesis of all classes of hormonal steroids. C(27) 3beta-HSD is a membrane-bound enzyme of the endoplasmic reticulum, it catalyzes the isomerization and oxidation of 7alpha-hydroxylated sterol intermediates, an early step in bile acid biosynthesis. Mutations in the human gene encoding C(27) 3beta-HSD underlie a rare autosomal recessive form of neonatal cholestasis. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid sythase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187671 [Multi-domain]  Cd Length: 354  Bit Score: 274.38  E-value: 1.15e-92
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  11 VYLVTGGCGFLGEHVVRMLLQREPRLGELRVFDQHLGPWLEELK---TGPVRVTAIQGDVTQAHEVAAAVAGAHVVIHTA 87
Cdd:cd09811     1 VCLVTGGGGFLGQHIIRLLLERKEELKEIRVLDKAFGPELIEHFeksQGKTYVTDIEGDIKDLSFLFRACQGVSVVIHTA 80
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  88 GLVDVFGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKGHPFYRGNEDTPYEAVHRHPYPCSKALAE 167
Cdd:cd09811    81 AIVDVFGPPNYEELEEVNVNGTQAVLEACVQNNVKRLVYTSSIEVAGPNFKGRPIFNGVEDTPYEDTSTPPYASSKLLAE 160
                         170
                  ....*....|
gi 1034596152 168 WLVLEANGRK 177
Cdd:cd09811   161 NIVLNANGAP 170
3Beta_HSD pfam01073
3-beta hydroxysteroid dehydrogenase/isomerase family; The enzyme 3 beta-hydroxysteroid ...
13-185 6.32e-64

3-beta hydroxysteroid dehydrogenase/isomerase family; The enzyme 3 beta-hydroxysteroid dehydrogenase/5-ene-4-ene isomerase (3 beta-HSD) catalyzes the oxidation and isomerization of 5-ene-3 beta-hydroxypregnene and 5-ene-hydroxyandrostene steroid precursors into the corresponding 4-ene-ketosteroids necessary for the formation of all classes of steroid hormones.


Pssm-ID: 366449 [Multi-domain]  Cd Length: 279  Bit Score: 198.74  E-value: 6.32e-64
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREPrLGELRVFDQHLGPWLEELKTGPVRVTAIQGDVTQAHEVAAAVAGAHVVIHTAGLVDV 92
Cdd:pfam01073   1 VVTGGGGFLGRHIIKLLVREGE-LKEVRVFDLRESPELLEDFSKSNVIKYIQGDVTDKDDLDNALEGVDVVIHTASAVDV 79
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  93 FGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKGHPFYRGNEDTPYEAVHRHPYPCSKALAEWLVLE 172
Cdd:pfam01073  80 FGKYTFDEIMKVNVKGTQNVLEACVKAGVRVLVYTSSAEVVGPNSYGQPILNGDEETPYESTHQDAYPRSKAIAEKLVLK 159
                         170
                  ....*....|....*
gi 1034596152 173 ANGRKAMLPG--CTC 185
Cdd:pfam01073 160 ANGRPLKNGGrlYTC 174
WcaG COG0451
Nucleoside-diphosphate-sugar epimerase [Cell wall/membrane/envelope biogenesis];
13-173 8.54e-29

Nucleoside-diphosphate-sugar epimerase [Cell wall/membrane/envelope biogenesis];


Pssm-ID: 440220 [Multi-domain]  Cd Length: 295  Bit Score: 108.53  E-value: 8.54e-29
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQReprlG-ELRVFDqHLGPWLEELKTGPvRVTAIQGDVTQAHEVAAAVAGAHVVIHTAGLVD 91
Cdd:COG0451     3 LVTGGAGFIGSHLARRLLAR----GhEVVGLD-RSPPGAANLAALP-GVEFVRGDLRDPEALAAALAGVDAVVHLAAPAG 76
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  92 VfGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNtkGHPFyrgNEDTPYEAvhRHPYPCSKALAEWLVL 171
Cdd:COG0451    77 V-GEEDPDETLEVNVEGTLNLLEAARAAGVKRFVYASSSSVYGDG--EGPI---DEDTPLRP--VSPYGASKLAAELLAR 148

                  ..
gi 1034596152 172 EA 173
Cdd:COG0451   149 AY 150
Thioester-redct TIGR01746
thioester reductase domain; This model includes the terminal domain from the fungal alpha ...
13-184 1.09e-13

thioester reductase domain; This model includes the terminal domain from the fungal alpha aminoadipate reductase enzyme (also known as aminoadipate semialdehyde dehydrogenase) which is involved in the biosynthesis of lysine, as well as the reductase-containing component of the myxochelin biosynthetic gene cluster, MxcG. The mechanism of reduction involves activation of the substrate by adenylation and transfer to a covalently-linked pantetheine cofactor as a thioester. This thioester is then reduced to give an aldehyde (thus releasing the product) and a regenerated pantetheine thiol. (In myxochelin biosynthesis this aldehyde is further reduced to an alcohol or converted to an amine by an aminotransferase.) This is a fundamentally different reaction than beta-ketoreductase domains of polyketide synthases which act at a carbonyl two carbons removed from the thioester and forms an alcohol as a product. This domain is invariably found at the C-terminus of the proteins which contain it (presumably because it results in the release of the product). The majority of hits to this model are non-ribosomal peptide synthetases in which this domain is similarly located proximal to a thiolation domain (pfam00550). In some cases this domain is found at the end of a polyketide synthetase enzyme, but is unlike ketoreductase domains which are found before the thiolase domains. Exceptions to this observed relationship with the thiolase domain include three proteins which consist of stand-alone reductase domains (GP|466833 from M. leprae, GP|435954 from Anabaena and OMNI|NTL02SC1199 from Strep. coelicolor) and one protein (OMNI|NTL01NS2636 from Nostoc) which contains N-terminal homology with a small group of hypothetical proteins but no evidence of a thiolation domain next to the putative reductase domain. Below the noise cutoff to this model are proteins containing more distantly related ketoreductase and dehydratase/epimerase domains. It has been suggested that a NADP-binding motif can be found in the N-terminal portion of this domain that may form a Rossman-type fold.


Pssm-ID: 273787 [Multi-domain]  Cd Length: 367  Bit Score: 68.21  E-value: 1.09e-13
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREPRLG---------------ELR-VFDQHLgpwLEELKTGPVRVTAIQGDVTQAHEVAAA 76
Cdd:TIGR01746   3 LLTGATGFLGAYLLEELLRRSTRAKviclvradseehameRLReALRSYR---LWHENLAMERIEVVAGDLSKPRLGLSD 79
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  77 VAGAHVV------IHTAGLVDVFGRASpkTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMeVVGPNTKGHPFYRGNED-- 148
Cdd:TIGR01746  80 AEWERLAenvdtiVHNGALVNHVYPYS--ELRGANVLGTVEVLRLAASGRAKPLHYVSTI-SVGAAIDLSTGVTEDDAtv 156
                         170       180       190
                  ....*....|....*....|....*....|....*.
gi 1034596152 149 TPYEAVHrHPYPCSKALAEWLVLEANGRKamLPGCT 184
Cdd:TIGR01746 157 TPYPGLA-GGYTQSKWVAELLVREASDRG--LPVTI 189
PRK07201 PRK07201
SDR family oxidoreductase;
12-182 8.61e-13

SDR family oxidoreductase;


Pssm-ID: 235962 [Multi-domain]  Cd Length: 657  Bit Score: 66.13  E-value: 8.61e-13
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREP--------RLGELRVFDQHLGPWleelktGPVRVTAIQGDVTQAHEVAAAVAGAHVV 83
Cdd:PRK07201    3 YFVTGGTGFIGRRLVSRLLDRRReatvhvlvRRQSLSRLEALAAYW------GADRVVPLVGDLTEPGLGLSEADIAELG 76
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  84 -----IHTAGLVDVfgRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGpntkghpFYRG--NEDTPYEAVH- 155
Cdd:PRK07201   77 didhvVHLAAIYDL--TADEEAQRAANVDGTRNVVELAERLQAATFHHVSSIAVAG-------DYEGvfREDDFDEGQGl 147
                         170       180       190
                  ....*....|....*....|....*....|...
gi 1034596152 156 RHPYPCSKALAEWLVLEANG------RKAMLPG 182
Cdd:PRK07201  148 PTPYHRTKFEAEKLVREECGlpwrvyRPAVVVG 180
PKS_KR smart00822
This enzymatic domain is part of bacterial polyketide synthases; It catalyses the first step ...
11-130 2.74e-07

This enzymatic domain is part of bacterial polyketide synthases; It catalyses the first step in the reductive modification of the beta-carbonyl centres in the growing polyketide chain. It uses NADPH to reduce the keto group to a hydroxy group.


Pssm-ID: 214833 [Multi-domain]  Cd Length: 180  Bit Score: 48.63  E-value: 2.74e-07
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152   11 VYLVTGGCGFLGEHVVRMLLQREPRlgelrvfdqHL------GP-------WLEELKTGPVRVTAIQGDVTQAHEVAAAV 77
Cdd:smart00822   2 TYLITGGLGGLGRALARWLAERGAR---------RLvllsrsGPdapgaaaLLAELEAAGARVTVVACDVADRDALAAVL 72
                           90       100       110       120       130       140
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*
gi 1034596152   78 AGAHVV-------IHTAGLVD--VFGRASPKTIHEVN---VQGTRNVIEACVQTGTRFLVYTSSM 130
Cdd:smart00822  73 AAIPAVegpltgvIHAAGVLDdgVLASLTPERFAAVLapkAAGAWNLHELTADLPLDFFVLFSSI 137
 
Name Accession Description Interval E-value
3b-HSD_HSDB1_like_SDR_e cd09811
human 3beta-HSD (hydroxysteroid dehydrogenase) and HSD3B1(delta 5-delta 4-isomerase)-like, ...
11-177 1.15e-92

human 3beta-HSD (hydroxysteroid dehydrogenase) and HSD3B1(delta 5-delta 4-isomerase)-like, extended (e) SDRs; This extended-SDR subgroup includes human 3 beta-HSD/HSD3B1 and C(27) 3beta-HSD/ [3beta-hydroxy-delta(5)-C(27)-steroid oxidoreductase; HSD3B7], and related proteins. These proteins have the characteristic active site tetrad and NAD(P)-binding motif of extended SDRs. 3 beta-HSD catalyzes the oxidative conversion of delta 5-3 beta-hydroxysteroids to the delta 4-3-keto configuration; this activity is essential for the biosynthesis of all classes of hormonal steroids. C(27) 3beta-HSD is a membrane-bound enzyme of the endoplasmic reticulum, it catalyzes the isomerization and oxidation of 7alpha-hydroxylated sterol intermediates, an early step in bile acid biosynthesis. Mutations in the human gene encoding C(27) 3beta-HSD underlie a rare autosomal recessive form of neonatal cholestasis. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid sythase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187671 [Multi-domain]  Cd Length: 354  Bit Score: 274.38  E-value: 1.15e-92
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  11 VYLVTGGCGFLGEHVVRMLLQREPRLGELRVFDQHLGPWLEELK---TGPVRVTAIQGDVTQAHEVAAAVAGAHVVIHTA 87
Cdd:cd09811     1 VCLVTGGGGFLGQHIIRLLLERKEELKEIRVLDKAFGPELIEHFeksQGKTYVTDIEGDIKDLSFLFRACQGVSVVIHTA 80
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  88 GLVDVFGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKGHPFYRGNEDTPYEAVHRHPYPCSKALAE 167
Cdd:cd09811    81 AIVDVFGPPNYEELEEVNVNGTQAVLEACVQNNVKRLVYTSSIEVAGPNFKGRPIFNGVEDTPYEDTSTPPYASSKLLAE 160
                         170
                  ....*....|
gi 1034596152 168 WLVLEANGRK 177
Cdd:cd09811   161 NIVLNANGAP 170
3Beta_HSD pfam01073
3-beta hydroxysteroid dehydrogenase/isomerase family; The enzyme 3 beta-hydroxysteroid ...
13-185 6.32e-64

3-beta hydroxysteroid dehydrogenase/isomerase family; The enzyme 3 beta-hydroxysteroid dehydrogenase/5-ene-4-ene isomerase (3 beta-HSD) catalyzes the oxidation and isomerization of 5-ene-3 beta-hydroxypregnene and 5-ene-hydroxyandrostene steroid precursors into the corresponding 4-ene-ketosteroids necessary for the formation of all classes of steroid hormones.


Pssm-ID: 366449 [Multi-domain]  Cd Length: 279  Bit Score: 198.74  E-value: 6.32e-64
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREPrLGELRVFDQHLGPWLEELKTGPVRVTAIQGDVTQAHEVAAAVAGAHVVIHTAGLVDV 92
Cdd:pfam01073   1 VVTGGGGFLGRHIIKLLVREGE-LKEVRVFDLRESPELLEDFSKSNVIKYIQGDVTDKDDLDNALEGVDVVIHTASAVDV 79
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  93 FGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKGHPFYRGNEDTPYEAVHRHPYPCSKALAEWLVLE 172
Cdd:pfam01073  80 FGKYTFDEIMKVNVKGTQNVLEACVKAGVRVLVYTSSAEVVGPNSYGQPILNGDEETPYESTHQDAYPRSKAIAEKLVLK 159
                         170
                  ....*....|....*
gi 1034596152 173 ANGRKAMLPG--CTC 185
Cdd:pfam01073 160 ANGRPLKNGGrlYTC 174
3b-HSD-like_SDR_e cd05241
3beta-hydroxysteroid dehydrogenases (3b-HSD)-like, extended (e) SDRs; Extended SDR family ...
13-185 5.55e-37

3beta-hydroxysteroid dehydrogenases (3b-HSD)-like, extended (e) SDRs; Extended SDR family domains belonging to this subgroup have the characteristic active site tetrad and a fairly well-conserved NAD(P)-binding motif. 3b-HSD catalyzes the NAD-dependent conversion of various steroids, such as pregnenolone to progesterone, or androstenediol to testosterone. This subgroup includes an unusual bifunctional 3b-HSD/C-4 decarboxylase from Arabidopsis thaliana, and Saccharomyces cerevisiae ERG26, a 3b-HSD/C-4 decarboxylase, involved in the synthesis of ergosterol, the major sterol of yeast. It also includes human 3 beta-HSD/HSD3B1 and C(27) 3beta-HSD/ [3beta-hydroxy-delta(5)-C(27)-steroid oxidoreductase; HSD3B7]. C(27) 3beta-HSD/HSD3B7 is a membrane-bound enzyme of the endoplasmic reticulum, that catalyzes the isomerization and oxidation of 7alpha-hydroxylated sterol intermediates, an early step in bile acid biosynthesis. Mutations in the human NSDHL (NAD(P)H steroid dehydrogenase-like protein) cause CHILD syndrome (congenital hemidysplasia with ichthyosiform nevus and limb defects), an X-linked dominant, male-lethal trait. Mutations in the human gene encoding C(27) 3beta-HSD underlie a rare autosomal recessive form of neonatal cholestasis. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid sythase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187552 [Multi-domain]  Cd Length: 331  Bit Score: 130.63  E-value: 5.55e-37
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREprLGELRVFDqhLGPWLEEL-KTGPVRVTAIQGDVTQAHEVAAAVAGAHVVIHTAGLVD 91
Cdd:cd05241     3 LVTGGSGFFGERLVKQLLERG--GTYVRSFD--IAPPGEALsAWQHPNIEFLKGDITDRNDVEQALSGADCVFHTAAIVP 78
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  92 VFGrasPKTIH-EVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPntkGHPFYRGNEDTPYEAVHRHPYPCSKALAEWLV 170
Cdd:cd05241    79 LAG---PRDLYwEVNVGGTQNVLDACQRCGVQKFVYTSSSSVIFG---GQNIHNGDETLPYPPLDSDMYAETKAIAEIIV 152
                         170
                  ....*....|....*
gi 1034596152 171 LEANGRKAMLpgcTC 185
Cdd:cd05241   153 LEANGRDDLL---TC 164
3b-HSD-NSDHL-like_SDR_e cd09813
human NSDHL (NAD(P)H steroid dehydrogenase-like protein)-like, extended (e) SDRs; This ...
12-183 6.94e-36

human NSDHL (NAD(P)H steroid dehydrogenase-like protein)-like, extended (e) SDRs; This subgroup includes human NSDHL and related proteins. These proteins have the characteristic active site tetrad of extended SDRs, and also have a close match to their NAD(P)-binding motif. Human NSDHL is a 3beta-hydroxysteroid dehydrogenase (3 beta-HSD) which functions in the cholesterol biosynthetic pathway. 3 beta-HSD catalyzes the oxidative conversion of delta 5-3 beta-hydroxysteroids to the delta 4-3-keto configuration; this activity is essential for the biosynthesis of all classes of hormonal steroids. Mutations in the gene encoding NSDHL cause CHILD syndrome (congenital hemidysplasia with ichthyosiform nevus and limb defects), an X-linked dominant, male-lethal trait. This subgroup also includes an unusual bifunctional [3beta-hydroxysteroid dehydrogenase (3b-HSD)/C-4 decarboxylase from Arabidopsis thaliana, and Saccharomyces cerevisiae ERG26, a 3b-HSD/C-4 decarboxylase, involved in the synthesis of ergosterol, the major sterol of yeast. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid sythase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187673 [Multi-domain]  Cd Length: 335  Bit Score: 127.86  E-value: 6.94e-36
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREPRlgELRVFDqhLGPWLEELKTGPVRVTAIQGDVT--QAHEVAAAVAGAHVVIHTAGL 89
Cdd:cd09813     2 CLVVGGSGFLGRHLVEQLLRRGNP--TVHVFD--IRPTFELDPSSSGRVQFHTGDLTdpQDLEKAFNEKGPNVVFHTASP 77
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  90 VDVFGRAspkTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVgpnTKGHPFYRGNEDTPYEAVHRHPYPCSKALAEWL 169
Cdd:cd09813    78 DHGSNDD---LYYKVNVQGTRNVIEACRKCGVKKLVYTSSASVV---FNGQDIINGDESLPYPDKHQDAYNETKALAEKL 151
                         170
                  ....*....|....
gi 1034596152 170 VLEANGRKAMLPGC 183
Cdd:cd09813   152 VLKANDPESGLLTC 165
WcaG COG0451
Nucleoside-diphosphate-sugar epimerase [Cell wall/membrane/envelope biogenesis];
13-173 8.54e-29

Nucleoside-diphosphate-sugar epimerase [Cell wall/membrane/envelope biogenesis];


Pssm-ID: 440220 [Multi-domain]  Cd Length: 295  Bit Score: 108.53  E-value: 8.54e-29
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQReprlG-ELRVFDqHLGPWLEELKTGPvRVTAIQGDVTQAHEVAAAVAGAHVVIHTAGLVD 91
Cdd:COG0451     3 LVTGGAGFIGSHLARRLLAR----GhEVVGLD-RSPPGAANLAALP-GVEFVRGDLRDPEALAAALAGVDAVVHLAAPAG 76
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  92 VfGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNtkGHPFyrgNEDTPYEAvhRHPYPCSKALAEWLVL 171
Cdd:COG0451    77 V-GEEDPDETLEVNVEGTLNLLEAARAAGVKRFVYASSSSVYGDG--EGPI---DEDTPLRP--VSPYGASKLAAELLAR 148

                  ..
gi 1034596152 172 EA 173
Cdd:COG0451   149 AY 150
AR_FR_like_1_SDR_e cd05228
uncharacterized subgroup of aldehyde reductase and flavonoid reductase related proteins, ...
13-173 1.82e-22

uncharacterized subgroup of aldehyde reductase and flavonoid reductase related proteins, extended (e) SDRs; This subgroup contains proteins of unknown function related to aldehyde reductase and flavonoid reductase of the extended SDR-type. Aldehyde reductase I (aka carbonyl reductase) is an NADP-binding SDR; it has an NADP-binding motif consensus that is slightly different from the canonical SDR form and lacks the Asn of the extended SDR active site tetrad. Aldehyde reductase I catalyzes the NADP-dependent reduction of ethyl 4-chloro-3-oxobutanoate to ethyl (R)-4-chloro-3-hydroxybutanoate. The related flavonoid reductases act in the NADP-dependent reduction of flavonoids, ketone-containing plant secondary metabolites. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187539 [Multi-domain]  Cd Length: 318  Bit Score: 91.96  E-value: 1.82e-22
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQReprlGE-LRVFDQHLGPwLEELKTGPVRVtaIQGDVTQAHEVAAAVAGAHVVIHTAGLVD 91
Cdd:cd05228     2 LVTGATGFLGSNLVRALLAQ----GYrVRALVRSGSD-AVLLDGLPVEV--VEGDLTDAASLAAAMKGCDRVFHLAAFTS 74
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  92 VFGRaSPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKGhpfyRGNEDTPYEAVHRH-PYPCSKALAEWLV 170
Cdd:cd05228    75 LWAK-DRKELYRTNVEGTRNVLDAALEAGVRRVVHTSSIAALGGPPDG----RIDETTPWNERPFPnDYYRSKLLAELEV 149

                  ...
gi 1034596152 171 LEA 173
Cdd:cd05228   150 LEA 152
UDP_AE_SDR_e cd05256
UDP-N-acetylglucosamine 4-epimerase, extended (e) SDRs; This subgroup contains ...
12-167 1.97e-20

UDP-N-acetylglucosamine 4-epimerase, extended (e) SDRs; This subgroup contains UDP-N-acetylglucosamine 4-epimerase of Pseudomonas aeruginosa, WbpP, an extended SDR, that catalyzes the NAD+ dependent conversion of UDP-GlcNAc and UDPGalNA to UDP-Glc and UDP-Gal. This subgroup has the characteristic active site tetrad and NAD-binding motif of the extended SDRs. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187566 [Multi-domain]  Cd Length: 304  Bit Score: 86.50  E-value: 1.97e-20
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREprlGELRVFDQHLGPWLEELKTGPVRVTAIQGDVTQAHEVAAAVAGAHVVIHTAGLVD 91
Cdd:cd05256     2 VLVTGGAGFIGSHLVERLLERG---HEVIVLDNLSTGKKENLPEVKPNVKFIEGDIRDDELVEFAFEGVDYVFHQAAQAS 78
                          90       100       110       120       130       140       150
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....
gi 1034596152  92 VfgRAS---PKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGpntkGHPFYRGNEDTPYEAVhrHPYPCSKALAE 167
Cdd:cd05256    79 V--PRSiedPIKDHEVNVLGTLNLLEAARKAGVKRFVYASSSSVYG----DPPYLPKDEDHPPNPL--SPYAVSKYAGE 149
SDR_e cd08946
extended (e) SDRs; Extended SDRs are distinct from classical SDRs. In addition to the Rossmann ...
12-172 3.42e-19

extended (e) SDRs; Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 212494 [Multi-domain]  Cd Length: 200  Bit Score: 81.19  E-value: 3.42e-19
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREPrlgELRVFDqhlgpwleelktgpvRVTAIqgdvtqahevaaavagahvvIHTAGLVD 91
Cdd:cd08946     1 ILVTGGAGFIGSHLVRRLLERGH---EVVVID---------------RLDVV--------------------VHLAALVG 42
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  92 V-FGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKghpfyrGNEDTPYEAVHRHPYPCSKALAEWLV 170
Cdd:cd08946    43 VpASWDNPDEDFETNVVGTLNLLEAARKAGVKRFVYASSASVYGSPEG------LPEEEETPPRPLSPYGVSKLAAEHLL 116

                  ..
gi 1034596152 171 LE 172
Cdd:cd08946   117 RS 118
MupV_like_SDR_e cd05263
Pseudomonas fluorescens MupV-like, extended (e) SDRs; This subgroup of extended SDR family ...
12-173 2.00e-17

Pseudomonas fluorescens MupV-like, extended (e) SDRs; This subgroup of extended SDR family domains have the characteristic active site tetrad and a well-conserved NAD(P)-binding motif. This subgroup is not well characterized, its members are annotated as having a variety of putative functions. One characterized member is Pseudomonas fluorescens MupV a protein involved in the biosynthesis of Mupirocin, a polyketide-derived antibiotic. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187573 [Multi-domain]  Cd Length: 293  Bit Score: 78.18  E-value: 2.00e-17
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREprlGELRVF-----DQHLGPWLEELKTGPVRVTAIQGDVTQ------AHEVAAAVAGA 80
Cdd:cd05263     1 VFVTGGTGFLGRHLVKRLLENG---FKVLVLvrsesLGEAHERIEEAGLEADRVRVLEGDLTQpnlglsAAASRELAGKV 77
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  81 HVVIHTAGLVDVfgRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTkGHpfYRGNEDTPYEAVHrHPYP 160
Cdd:cd05263    78 DHVIHCAASYDF--QAPNEDAWRTNIDGTEHVLELAARLDIQRFHYVSTAYVAGNRE-GN--IRETELNPGQNFK-NPYE 151
                         170
                  ....*....|...
gi 1034596152 161 CSKALAEWLVLEA 173
Cdd:cd05263   152 QSKAEAEQLVRAA 164
RfbB COG1088
dTDP-D-glucose 4,6-dehydratase [Cell wall/membrane/envelope biogenesis];
12-171 3.07e-16

dTDP-D-glucose 4,6-dehydratase [Cell wall/membrane/envelope biogenesis];


Pssm-ID: 440705 [Multi-domain]  Cd Length: 333  Bit Score: 75.12  E-value: 3.07e-16
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREPRLgELRVFDQ-----HLGpWLEELKTGPvRVTAIQGDVTQAHEVAAAVAGAHVV--I 84
Cdd:COG1088     4 ILVTGGAGFIGSNFVRYLLAKYPGA-EVVVLDKltyagNLE-NLADLEDDP-RYRFVKGDIRDRELVDELFAEHGPDavV 80
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  85 HTAGL--VDvfgR--ASPKTIHEVNVQGTRNVIEACVQTGT---RFlVYTSSMEVVGPNTKGHPFyrgNEDTPYEAvhRH 157
Cdd:COG1088    81 HFAAEshVD---RsiDDPAAFVETNVVGTFNLLEAARKYWVegfRF-HHVSTDEVYGSLGEDGPF---TETTPLDP--SS 151
                         170
                  ....*....|....
gi 1034596152 158 PYPCSKALAEWLVL 171
Cdd:COG1088   152 PYSASKAASDHLVR 165
Epimerase pfam01370
NAD dependent epimerase/dehydratase family; This family of proteins utilize NAD as a cofactor. ...
13-174 5.85e-16

NAD dependent epimerase/dehydratase family; This family of proteins utilize NAD as a cofactor. The proteins in this family use nucleotide-sugar substrates for a variety of chemical reactions.


Pssm-ID: 396097 [Multi-domain]  Cd Length: 238  Bit Score: 73.10  E-value: 5.85e-16
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREPrlgELRVFDqHLGPWLEELKTGPVRVtaIQGDVTQAHEVAAAVAGAH--VVIHTAGLV 90
Cdd:pfam01370   2 LVTGATGFIGSHLVRRLLEKGY---EVIGLD-RLTSASNTARLADLRF--VEGDLTDRDALEKLLADVRpdAVIHLAAVG 75
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  91 DVFGRAS-PKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKGhpfyRGNEDTPYEAVHRH-PYPCSKALAEW 168
Cdd:pfam01370  76 GVGASIEdPEDFIEANVLGTLNLLEAARKAGVKRFLFASSSEVYGDGAEI----PQEETTLTGPLAPNsPYAAAKLAGEW 151

                  ....*.
gi 1034596152 169 LVLEAN 174
Cdd:pfam01370 152 LVLAYA 157
Lys2b COG3320
Thioester reductase domain of alpha aminoadipate reductase Lys2 and NRPSs [Secondary ...
11-177 7.95e-16

Thioester reductase domain of alpha aminoadipate reductase Lys2 and NRPSs [Secondary metabolites biosynthesis, transport and catabolism]; Thioester reductase domain of alpha aminoadipate reductase Lys2 and NRPSs is part of the Pathway/BioSystem: Lysine biosynthesis


Pssm-ID: 442549 [Multi-domain]  Cd Length: 265  Bit Score: 73.32  E-value: 7.95e-16
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  11 VYLVTGGCGFLGEHVVRMLLQREP-----------------RLGELRvfdQHLGPWLEELKTgpvRVTAIQGDVTQ---- 69
Cdd:COG3320     2 TVLLTGATGFLGAHLLRELLRRTDarvyclvrasdeaaareRLEALL---ERYGLWLELDAS---RVVVVAGDLTQprlg 75
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  70 --AHEVAAAVAGAHVVIHTAGLVDVFgrASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTkgHPFYRGNE 147
Cdd:COG3320    76 lsEAEFQELAEEVDAIVHLAALVNLV--APYSELRAVNVLGTREVLRLAATGRLKPFHYVSTIAVAGPAD--RSGVFEED 151
                         170       180       190
                  ....*....|....*....|....*....|
gi 1034596152 148 DTPYEAVHRHPYPCSKALAEWLVLEANGRK 177
Cdd:COG3320   152 DLDEGQGFANGYEQSKWVAEKLVREARERG 181
3b-HSD_like_1_SDR_e cd09812
3beta-hydroxysteroid dehydrogenase (3b-HSD)-like, subgroup1, extended (e) SDRs; An ...
13-175 1.58e-15

3beta-hydroxysteroid dehydrogenase (3b-HSD)-like, subgroup1, extended (e) SDRs; An uncharacterized subgroup of the 3b-HSD-like extended-SDR family. Proteins in this subgroup have the characteristic active site tetrad and NAD(P)-binding motif of extended-SDRs. 3 beta-HSD catalyzes the oxidative conversion of delta 5-3 beta-hydroxysteroids to the delta 4-3-keto configuration; this activity is essential for the biosynthesis of all classes of hormonal steroids. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid sythase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187672 [Multi-domain]  Cd Length: 339  Bit Score: 73.31  E-value: 1.58e-15
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREPR--LGELRVFDQHLgpwleelktgPVRVTAIQGDVTQAHEVAAAVAGAHVVIHTAGLv 90
Cdd:cd09812     3 LITGGGGYFGFRLGCALAKSGVHviLFDIRRPQQEL----------PEGIKFIQADVRDLSQLEKAVAGVDCVFHIASY- 71
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  91 DVFGRA--SPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVgpnTKGHPFYRGNEDTPYEAVHRHP--YPCSKALA 166
Cdd:cd09812    72 GMSGREqlNRELIEEINVRGTENIIQVCVRRRVPRLIYTSTFNVI---FGGQPIRNGDESLPYLPLDLHVdhYSRTKSIA 148

                  ....*....
gi 1034596152 167 EWLVLEANG 175
Cdd:cd09812   149 EQLVLKANN 157
Arna_like_SDR_e cd05257
Arna decarboxylase_like, extended (e) SDRs; Decarboxylase domain of ArnA. ArnA, is an enzyme ...
13-181 2.62e-15

Arna decarboxylase_like, extended (e) SDRs; Decarboxylase domain of ArnA. ArnA, is an enzyme involved in the modification of outer membrane protein lipid A of gram-negative bacteria. It is a bifunctional enzyme that catalyzes the NAD-dependent decarboxylation of UDP-glucuronic acid and N-10-formyltetrahydrofolate-dependent formylation of UDP-4-amino-4-deoxy-l-arabinose; its NAD-dependent decaboxylating activity is in the C-terminal 360 residues. This subgroup belongs to the extended SDR family, however the NAD binding motif is not a perfect match and the upstream Asn of the canonical active site tetrad is not conserved. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187567 [Multi-domain]  Cd Length: 316  Bit Score: 72.33  E-value: 2.62e-15
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLqrepRLG-ELRVFDQH--LGPWLEELKTGPVRVTAIQGDVTQAHEVAAAVAGAHVVIHTAGL 89
Cdd:cd05257     3 LVTGADGFIGSHLTERLL----REGhEVRALDIYnsFNSWGLLDNAVHDRFHFISGDVRDASEVEYLVKKCDVVFHLAAL 78
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  90 VDV-FGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGpntKGHPFYRGnEDTP--YEAVHRHPYPCSKALA 166
Cdd:cd05257    79 IAIpYSYTAPLSYVETNVFGTLNVLEAACVLYRKRVVHTSTSEVYG---TAQDVPID-EDHPllYINKPRSPYSASKQGA 154
                         170
                  ....*....|....*
gi 1034596152 167 EWLVlEANGRKAMLP 181
Cdd:cd05257   155 DRLA-YSYGRSFGLP 168
CDP_TE_SDR_e cd05258
CDP-tyvelose 2-epimerase, extended (e) SDRs; CDP-tyvelose 2-epimerase is a tetrameric SDR that ...
11-172 7.55e-15

CDP-tyvelose 2-epimerase, extended (e) SDRs; CDP-tyvelose 2-epimerase is a tetrameric SDR that catalyzes the conversion of CDP-D-paratose to CDP-D-tyvelose, the last step in tyvelose biosynthesis. This subgroup is a member of the extended SDR subfamily, with a characteristic active site tetrad and NAD-binding motif. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187568 [Multi-domain]  Cd Length: 337  Bit Score: 71.17  E-value: 7.55e-15
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  11 VYLVTGGCGFLGEHVVRMLLQREprlGELRVFDQHL-------GPWLEELKTGPvRVTAIQGDVTQAHEVAAAVAGAHVV 83
Cdd:cd05258     2 RVLITGGAGFIGSNLARFFLKQG---WEVIGFDNLMrrgsfgnLAWLKANREDG-GVRFVHGDIRNRNDLEDLFEDIDLI 77
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  84 IHTAGLVDV-FGRASPKTIHEVNVQGTRNVIEACVQTGTR-FLVYTSSMEVVGPNTKGHPFYRG------NEDTPYEA-- 153
Cdd:cd05258    78 IHTAAQPSVtTSASSPRLDFETNALGTLNVLEAARQHAPNaPFIFTSTNKVYGDLPNYLPLEELetryelAPEGWSPAgi 157
                         170       180
                  ....*....|....*....|....*.
gi 1034596152 154 -------VHRHPYPCSKALAEWLVLE 172
Cdd:cd05258   158 sesfpldFSHSLYGASKGAADQYVQE 183
Thioester-redct TIGR01746
thioester reductase domain; This model includes the terminal domain from the fungal alpha ...
13-184 1.09e-13

thioester reductase domain; This model includes the terminal domain from the fungal alpha aminoadipate reductase enzyme (also known as aminoadipate semialdehyde dehydrogenase) which is involved in the biosynthesis of lysine, as well as the reductase-containing component of the myxochelin biosynthetic gene cluster, MxcG. The mechanism of reduction involves activation of the substrate by adenylation and transfer to a covalently-linked pantetheine cofactor as a thioester. This thioester is then reduced to give an aldehyde (thus releasing the product) and a regenerated pantetheine thiol. (In myxochelin biosynthesis this aldehyde is further reduced to an alcohol or converted to an amine by an aminotransferase.) This is a fundamentally different reaction than beta-ketoreductase domains of polyketide synthases which act at a carbonyl two carbons removed from the thioester and forms an alcohol as a product. This domain is invariably found at the C-terminus of the proteins which contain it (presumably because it results in the release of the product). The majority of hits to this model are non-ribosomal peptide synthetases in which this domain is similarly located proximal to a thiolation domain (pfam00550). In some cases this domain is found at the end of a polyketide synthetase enzyme, but is unlike ketoreductase domains which are found before the thiolase domains. Exceptions to this observed relationship with the thiolase domain include three proteins which consist of stand-alone reductase domains (GP|466833 from M. leprae, GP|435954 from Anabaena and OMNI|NTL02SC1199 from Strep. coelicolor) and one protein (OMNI|NTL01NS2636 from Nostoc) which contains N-terminal homology with a small group of hypothetical proteins but no evidence of a thiolation domain next to the putative reductase domain. Below the noise cutoff to this model are proteins containing more distantly related ketoreductase and dehydratase/epimerase domains. It has been suggested that a NADP-binding motif can be found in the N-terminal portion of this domain that may form a Rossman-type fold.


Pssm-ID: 273787 [Multi-domain]  Cd Length: 367  Bit Score: 68.21  E-value: 1.09e-13
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREPRLG---------------ELR-VFDQHLgpwLEELKTGPVRVTAIQGDVTQAHEVAAA 76
Cdd:TIGR01746   3 LLTGATGFLGAYLLEELLRRSTRAKviclvradseehameRLReALRSYR---LWHENLAMERIEVVAGDLSKPRLGLSD 79
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  77 VAGAHVV------IHTAGLVDVFGRASpkTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMeVVGPNTKGHPFYRGNED-- 148
Cdd:TIGR01746  80 AEWERLAenvdtiVHNGALVNHVYPYS--ELRGANVLGTVEVLRLAASGRAKPLHYVSTI-SVGAAIDLSTGVTEDDAtv 156
                         170       180       190
                  ....*....|....*....|....*....|....*.
gi 1034596152 149 TPYEAVHrHPYPCSKALAEWLVLEANGRKamLPGCT 184
Cdd:TIGR01746 157 TPYPGLA-GGYTQSKWVAELLVREASDRG--LPVTI 189
UDP_G4E_3_SDR_e cd05240
UDP-glucose 4 epimerase (G4E), subgroup 3, extended (e) SDRs; Members of this bacterial ...
13-173 1.64e-13

UDP-glucose 4 epimerase (G4E), subgroup 3, extended (e) SDRs; Members of this bacterial subgroup are identified as possible sugar epimerases, such as UDP-glucose 4 epimerase. However, while the NAD(P)-binding motif is fairly well conserved, not all members retain the canonical active site tetrad of the extended SDRs. UDP-glucose 4 epimerase (aka UDP-galactose-4-epimerase), is a homodimeric extended SDR. It catalyzes the NAD-dependent conversion of UDP-galactose to UDP-glucose, the final step in Leloir galactose synthesis. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187551 [Multi-domain]  Cd Length: 306  Bit Score: 67.39  E-value: 1.64e-13
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQrEPRLGELRVFDQHLGPWleelktGPVRVTAIQGDVTQAHEVAAAVAGAH-VVIHTAGLVD 91
Cdd:cd05240     2 LVTGAAGGLGRLLARRLAA-SPRVIGVDGLDRRRPPG------SPPKVEYVRLDIRDPAAADVFREREAdAVVHLAFILD 74
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  92 vfGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKGHPFYRgnEDTPYEAVHRHPYPCSKALAEWLVL 171
Cdd:cd05240    75 --PPRDGAERHRINVDGTQNVLDACAAAGVPRVVVTSSVAVYGAHPDNPAPLT--EDAPLRGSPEFAYSRDKAEVEQLLA 150

                  ..
gi 1034596152 172 EA 173
Cdd:cd05240   151 EF 152
AR_like_SDR_e cd05193
aldehyde reductase, flavonoid reductase, and related proteins, extended (e) SDRs; This ...
13-175 7.12e-13

aldehyde reductase, flavonoid reductase, and related proteins, extended (e) SDRs; This subgroup contains aldehyde reductase and flavonoid reductase of the extended SDR-type and related proteins. Proteins in this subgroup have a complete SDR-type active site tetrad and a close match to the canonical extended SDR NADP-binding motif. Aldehyde reductase I (aka carbonyl reductase) is an NADP-binding SDR; it catalyzes the NADP-dependent reduction of ethyl 4-chloro-3-oxobutanoate to ethyl (R)-4-chloro-3-hydroxybutanoate. The related flavonoid reductases act in the NADP-dependent reduction of flavonoids, ketone-containing plant secondary metabolites. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187536 [Multi-domain]  Cd Length: 295  Bit Score: 65.33  E-value: 7.12e-13
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQR----------------EPRLGELRVFDQHLGPWLEELKTGPVRVTAIQGdvtqahevaaa 76
Cdd:cd05193     2 LVTGASGFVASHVVEQLLERgykvratvrdpskvkkVNHLLDLDAKPGRLELAVADLTDEQSFDEVIKG----------- 70
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  77 vagAHVVIHTAGLVDvFGRASPKTIHEVNVQGTRNVIEACVQTGT-RFLVYTSSMEVVGPNTKGHPFYRGNE----DTPY 151
Cdd:cd05193    71 ---CAGVFHVATPVS-FSSKDPNEVIKPAIGGTLNALKAAAAAKSvKRFVLTSSAGSVLIPKPNVEGIVLDEkswnLEEF 146
                         170       180       190
                  ....*....|....*....|....*....|
gi 1034596152 152 EAVHRHP---YPCSKALAE---WLVLEANG 175
Cdd:cd05193   147 DSDPKKSawvYAASKTLAEkaaWKFADENN 176
PRK07201 PRK07201
SDR family oxidoreductase;
12-182 8.61e-13

SDR family oxidoreductase;


Pssm-ID: 235962 [Multi-domain]  Cd Length: 657  Bit Score: 66.13  E-value: 8.61e-13
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREP--------RLGELRVFDQHLGPWleelktGPVRVTAIQGDVTQAHEVAAAVAGAHVV 83
Cdd:PRK07201    3 YFVTGGTGFIGRRLVSRLLDRRReatvhvlvRRQSLSRLEALAAYW------GADRVVPLVGDLTEPGLGLSEADIAELG 76
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  84 -----IHTAGLVDVfgRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGpntkghpFYRG--NEDTPYEAVH- 155
Cdd:PRK07201   77 didhvVHLAAIYDL--TADEEAQRAANVDGTRNVVELAERLQAATFHHVSSIAVAG-------DYEGvfREDDFDEGQGl 147
                         170       180       190
                  ....*....|....*....|....*....|...
gi 1034596152 156 RHPYPCSKALAEWLVLEANG------RKAMLPG 182
Cdd:PRK07201  148 PTPYHRTKFEAEKLVREECGlpwrvyRPAVVVG 180
SDR_e1 cd05235
extended (e) SDRs, subgroup 1; This family consists of an SDR module of multidomain proteins ...
13-183 1.35e-12

extended (e) SDRs, subgroup 1; This family consists of an SDR module of multidomain proteins identified as putative polyketide sythases fatty acid synthases (FAS), and nonribosomal peptide synthases, among others. However, unlike the usual ketoreductase modules of FAS and polyketide synthase, these domains are related to the extended SDRs, and have canonical NAD(P)-binding motifs and an active site tetrad. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187546 [Multi-domain]  Cd Length: 290  Bit Score: 64.59  E-value: 1.35e-12
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREP------------------RLgeLRVFDQHLGPWLEELKTGpvRVTAIQGDVTQ----- 69
Cdd:cd05235     3 LLTGATGFLGAYLLRELLKRKNvskiyclvrakdeeaaleRL--IDNLKEYGLNLWDELELS--RIKVVVGDLSKpnlgl 78
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  70 -AHEVAAAVAGAHVVIHTAGLVDVFGRASpkTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKGHPFYRGNED 148
Cdd:cd05235    79 sDDDYQELAEEVDVIIHNGANVNWVYPYE--ELKPANVLGTKELLKLAATGKLKPLHFVSTLSVFSAEEYNALDDEESDD 156
                         170       180       190
                  ....*....|....*....|....*....|....*.
gi 1034596152 149 TPYEAV-HRHPYPCSKALAEWLVLEANGRkaMLPGC 183
Cdd:cd05235   157 MLESQNgLPNGYIQSKWVAEKLLREAANR--GLPVA 190
dTDP_GD_SDR_e cd05246
dTDP-D-glucose 4,6-dehydratase, extended (e) SDRs; This subgroup contains dTDP-D-glucose 4, ...
12-171 3.60e-12

dTDP-D-glucose 4,6-dehydratase, extended (e) SDRs; This subgroup contains dTDP-D-glucose 4,6-dehydratase and related proteins, members of the extended-SDR family, with the characteristic Rossmann fold core region, active site tetrad and NAD(P)-binding motif. dTDP-D-glucose 4,6-dehydratase is closely related to other sugar epimerases of the SDR family. dTDP-D-dlucose 4,6,-dehydratase catalyzes the second of four steps in the dTDP-L-rhamnose pathway (the dehydration of dTDP-D-glucose to dTDP-4-keto-6-deoxy-D-glucose) in the synthesis of L-rhamnose, a cell wall component of some pathogenic bacteria. In many gram negative bacteria, L-rhamnose is an important constituent of lipopoylsaccharide O-antigen. The larger N-terminal portion of dTDP-D-Glucose 4,6-dehydratase forms a Rossmann fold NAD-binding domain, while the C-terminus binds the sugar substrate. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187557 [Multi-domain]  Cd Length: 315  Bit Score: 63.72  E-value: 3.60e-12
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREPRlGELRVFD--------QHlgpwLEELKTGPvRVTAIQGDVTQAHEVAAAVAGAH-- 81
Cdd:cd05246     3 ILVTGGAGFIGSNFVRYLLNKYPD-YKIINLDkltyagnlEN----LEDVSSSP-RYRFVKGDICDAELVDRLFEEEKid 76
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  82 VVIHTAGL--VD-VFGRASPKTihEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKGHPFyrgNEDTPYEAvhRHP 158
Cdd:cd05246    77 AVIHFAAEshVDrSISDPEPFI--RTNVLGTYTLLEAARKYGVKRFVHISTDEVYGDLLDDGEF---TETSPLAP--TSP 149
                         170
                  ....*....|...
gi 1034596152 159 YPCSKALAEWLVL 171
Cdd:cd05246   150 YSASKAAADLLVR 162
UDP_G4E_2_SDR_e cd05234
UDP-glucose 4 epimerase, subgroup 2, extended (e) SDRs; UDP-glucose 4 epimerase (aka ...
12-167 5.57e-12

UDP-glucose 4 epimerase, subgroup 2, extended (e) SDRs; UDP-glucose 4 epimerase (aka UDP-galactose-4-epimerase), is a homodimeric extended SDR. It catalyzes the NAD-dependent conversion of UDP-galactose to UDP-glucose, the final step in Leloir galactose synthesis. This subgroup is comprised of archaeal and bacterial proteins, and has the characteristic active site tetrad and NAD-binding motif of the extended SDRs. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187545 [Multi-domain]  Cd Length: 305  Bit Score: 63.09  E-value: 5.57e-12
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREprlGELRVFD-----QHLGPWLEE-----------LKTGPVRVTAIQGDVTqahevaa 75
Cdd:cd05234     2 ILVTGGAGFIGSHLVDRLLEEG---NEVVVVDnlssgRRENIEPEFenkafrfvkrdLLDTADKVAKKDGDTV------- 71
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  76 avagahvvIHTAGLVDV-FGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVG-PNTKGHPfyrgnEDTPYea 153
Cdd:cd05234    72 --------FHLAANPDVrLGATDPDIDLEENVLATYNVLEAMRANGVKRIVFASSSTVYGeAKVIPTP-----EDYPP-- 136
                         170
                  ....*....|....*..
gi 1034596152 154 vhrHP---YPCSKALAE 167
Cdd:cd05234   137 ---LPisvYGASKLAAE 150
UDP_G4E_4_SDR_e cd05232
UDP-glucose 4 epimerase, subgroup 4, extended (e) SDRs; UDP-glucose 4 epimerase (aka ...
13-173 1.28e-11

UDP-glucose 4 epimerase, subgroup 4, extended (e) SDRs; UDP-glucose 4 epimerase (aka UDP-galactose-4-epimerase), is a homodimeric extended SDR. It catalyzes the NAD-dependent conversion of UDP-galactose to UDP-glucose, the final step in Leloir galactose synthesis. This subgroup is comprised of bacterial proteins, and includes the Staphylococcus aureus capsular polysaccharide Cap5N, which may have a role in the synthesis of UDP-N-acetyl-d-fucosamine. This subgroup has the characteristic active site tetrad and NAD-binding motif of the extended SDRs. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187543 [Multi-domain]  Cd Length: 303  Bit Score: 61.98  E-value: 1.28e-11
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQR--EPRLGELRVFDQHLGPWLEELKTgPVRVTAIQGDVTqahevaaavagahVVIHTAGLV 90
Cdd:cd05232     3 LVTGANGFIGRALVDKLLSRgeEVRIAVRNAENAEPSVVLAELPD-IDSFTDLFLGVD-------------AVVHLAARV 68
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  91 DVFGRASPKTI---HEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKGHPFyrgNEDTPyeAVHRHPYPCSKALAE 167
Cdd:cd05232    69 HVMNDQGADPLsdyRKVNTELTRRLARAAARQGVKRFVFLSSVKVNGEGTVGAPF---DETDP--PAPQDAYGRSKLEAE 143

                  ....*.
gi 1034596152 168 WLVLEA 173
Cdd:cd05232   144 RALLEL 149
AR_SDR_e cd05227
aldehyde reductase, extended (e) SDRs; This subgroup contains aldehyde reductase of the ...
13-182 8.03e-11

aldehyde reductase, extended (e) SDRs; This subgroup contains aldehyde reductase of the extended SDR-type and related proteins. Aldehyde reductase I (aka carbonyl reductase) is an NADP-binding SDR; it has an NADP-binding motif consensus that is slightly different from the canonical SDR form and lacks the Asn of the extended SDR active site tetrad. Aldehyde reductase I catalyzes the NADP-dependent reduction of ethyl 4-chloro-3-oxobutanoate to ethyl (R)-4-chloro-3-hydroxybutanoate. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187538 [Multi-domain]  Cd Length: 301  Bit Score: 59.59  E-value: 8.03e-11
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQR----------EPRLGELR-VFDQHLGPwlEELKTgpvrvtAIQGDVTQAHEVAAAVAGAH 81
Cdd:cd05227     3 LVTGATGFIASHIVEQLLKAgykvrgtvrsLSKSAKLKaLLKAAGYN--DRLEF------VIVDDLTAPNAWDEALKGVD 74
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  82 VVIHTAGLVDVFGRASPKTIHEVNVQGTRNVIEACVQTGT-RFLVYTSSMEVVG---PNTKGHPFYRG--NEDTPYEAVH 155
Cdd:cd05227    75 YVIHVASPFPFTGPDAEDDVIDPAVEGTLNVLEAAKAAGSvKRVVLTSSVAAVGdptAEDPGKVFTEEdwNDLTISKSNG 154
                         170       180       190
                  ....*....|....*....|....*....|....
gi 1034596152 156 RHPYPCSKALAE---WLVLEANGRK----AMLPG 182
Cdd:cd05227   155 LDAYIASKTLAEkaaWEFVKENKPKfeliTINPG 188
GalE COG1087
UDP-glucose 4-epimerase [Cell wall/membrane/envelope biogenesis];
13-169 2.48e-10

UDP-glucose 4-epimerase [Cell wall/membrane/envelope biogenesis];


Pssm-ID: 440704 [Multi-domain]  Cd Length: 328  Bit Score: 58.49  E-value: 2.48e-10
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQReprlG-ELRVFDqhlgpwleELKTG-----PVRVTAIQGDVTQahevaaavagahvvihT 86
Cdd:COG1087     4 LVTGGAGYIGSHTVVALLEA----GhEVVVLD--------NLSNGhreavPKGVPFVEGDLRD----------------R 55
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  87 AGLVDVFGRASPKT-IH------------------EVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGpNTKGHPFyrgNE 147
Cdd:COG1087    56 AALDRVFAEHDIDAvIHfaalkavgesvekplkyyRNNVVGTLNLLEAMREAGVKRFVFSSSAAVYG-EPESVPI---TE 131
                         170       180
                  ....*....|....*....|..
gi 1034596152 148 DTPYEAVhrHPYPCSKALAEWL 169
Cdd:COG1087   132 DAPTNPT--NPYGRSKLMVEQI 151
Gne_like_SDR_e cd05238
Escherichia coli Gne (a nucleoside-diphosphate-sugar 4-epimerase)-like, extended (e) SDRs; ...
13-176 3.07e-10

Escherichia coli Gne (a nucleoside-diphosphate-sugar 4-epimerase)-like, extended (e) SDRs; Nucleoside-diphosphate-sugar 4-epimerase has the characteristic active site tetrad and NAD-binding motif of the extended SDR, and is related to more specifically defined epimerases such as UDP-glucose 4 epimerase (aka UDP-galactose-4-epimerase), which catalyzes the NAD-dependent conversion of UDP-galactose to UDP-glucose, the final step in Leloir galactose synthesis. This subgroup includes Escherichia coli 055:H7 Gne, a UDP-GlcNAc 4-epimerase, essential for O55 antigen synthesis. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187549 [Multi-domain]  Cd Length: 305  Bit Score: 58.16  E-value: 3.07e-10
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREPRLgELRVFD--QHLGPwleelkTGPVRVTAIQGDVTQAHEVAAAVAGAHVV-IHTAGL 89
Cdd:cd05238     4 LITGASGFVGQRLAERLLSDVPNE-RLILIDvvSPKAP------SGAPRVTQIAGDLAVPALIEALANGRPDVvFHLAAI 76
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  90 VDVFGRASPKTIHEVNVQGTRNVIEACVQTG--TRFlVYTSSMEVVGPntkghPFYRGNEDTPyeavHRHP---YPCSKA 164
Cdd:cd05238    77 VSGGAEADFDLGYRVNVDGTRNLLEALRKNGpkPRF-VFTSSLAVYGL-----PLPNPVTDHT----ALDPassYGAQKA 146
                         170
                  ....*....|..
gi 1034596152 165 LAEWLVLEANGR 176
Cdd:cd05238   147 MCELLLNDYSRR 158
NAD_binding_4 pfam07993
Male sterility protein; This family represents the C-terminal region of the male sterility ...
14-183 3.88e-10

Male sterility protein; This family represents the C-terminal region of the male sterility protein in a number of arabidopsis and drosophila. A sequence-related jojoba acyl CoA reductase is also included.


Pssm-ID: 462334 [Multi-domain]  Cd Length: 257  Bit Score: 57.23  E-value: 3.88e-10
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  14 VTGGCGFLGEHVVRMLLQREPRLGEL--------------RVFD--QHLGPWLEELKTGPVRVTAIQGDVTQ------AH 71
Cdd:pfam07993   1 LTGATGFLGKVLLEKLLRSTPDVKKIyllvrakdgesaleRLRQelEKYPLFDALLKEALERIVPVAGDLSEpnlglsEE 80
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  72 EVAAAVAGAHVVIHTAGLVDVFGRAspKTIHEVNVQGTRNVIEACVQT-GTRFLVYTSSmEVVGPNTKGH---PFYRG-- 145
Cdd:pfam07993  81 DFQELAEEVDVIIHSAATVNFVEPY--DDARAVNVLGTREVLRLAKQGkQLKPFHHVST-AYVNGERGGLveeKPYPEge 157
                         170       180       190       200
                  ....*....|....*....|....*....|....*....|....
gi 1034596152 146 -----NEDTPYEAV-HRHPYPCSKALAEWLVLEANGRKamLPGC 183
Cdd:pfam07993 158 ddmllDEDEPALLGgLPNGYTQTKWLAEQLVREAARRG--LPVV 199
FR_SDR_e cd08958
flavonoid reductase (FR), extended (e) SDRs; This subgroup contains FRs of the extended ...
12-167 6.00e-10

flavonoid reductase (FR), extended (e) SDRs; This subgroup contains FRs of the extended SDR-type and related proteins. These FRs act in the NADP-dependent reduction of flavonoids, ketone-containing plant secondary metabolites; they have the characteristic active site triad of the SDRs (though not the upstream active site Asn) and a NADP-binding motif that is very similar to the typical extended SDR motif. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187661 [Multi-domain]  Cd Length: 293  Bit Score: 57.20  E-value: 6.00e-10
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQR-------------EPRLGELRVfdqhlgpwLEELKTgpvRVTAIQGDVTQAHEVAAAVA 78
Cdd:cd08958     1 VCVTGASGFIGSWLVKRLLQRgytvratvrdpgdEKKVAHLLE--------LEGAKE---RLKLFKADLLDYGSFDAAID 69
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  79 GAHVVIHTAGLVDVFGRASPKTIHEVNVQGTRNVIEACVQTGT-RFLVYTSSMEVVGPNTKGHP-------------FYR 144
Cdd:cd08958    70 GCDGVFHVASPVDFDSEDPEEEMIEPAVKGTLNVLEACAKAKSvKRVVFTSSVAAVVWNPNRGEgkvvdescwsdldFCK 149
                         170       180
                  ....*....|....*....|...
gi 1034596152 145 GNEDTpyeavhrhpYPCSKALAE 167
Cdd:cd08958   150 KTKLW---------YALSKTLAE 163
GDP_Man_Dehyd pfam16363
GDP-mannose 4,6 dehydratase;
13-171 2.70e-09

GDP-mannose 4,6 dehydratase;


Pssm-ID: 465104 [Multi-domain]  Cd Length: 327  Bit Score: 55.25  E-value: 2.70e-09
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREPRLGELRVFDQHLGPW-LEELKTGPV--RVTAIQGDVTqahevaaavagahvviHTAGL 89
Cdd:pfam16363   1 LITGITGQDGSYLAELLLEKGYEVHGIVRRSSSFNTGrLEHLYDDHLngNLVLHYGDLT----------------DSSNL 64
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  90 VDVFGRASPKTI-------H------------EVNVQGTRNVIEACVQTG----TRFLVyTSSMEVVGpNTKGHPFyrgN 146
Cdd:pfam16363  65 VRLLAEVQPDEIynlaaqsHvdvsfeqpeytaDTNVLGTLRLLEAIRSLGlekkVRFYQ-ASTSEVYG-KVQEVPQ---T 139
                         170       180
                  ....*....|....*....|....*
gi 1034596152 147 EDTPYEAvhRHPYPCSKALAEWLVL 171
Cdd:pfam16363 140 ETTPFYP--RSPYAAAKLYADWIVV 162
KR_2_SDR_x cd08953
ketoreductase (KR), subgroup 2, complex (x) SDRs; Ketoreductase, a module of the multidomain ...
11-130 1.64e-08

ketoreductase (KR), subgroup 2, complex (x) SDRs; Ketoreductase, a module of the multidomain polyketide synthase (PKS), has 2 subdomains, each corresponding to a SDR family monomer. The C-terminal subdomain catalyzes the NADPH-dependent reduction of the beta-carbonyl of a polyketide to a hydroxyl group, a step in the biosynthesis of polyketides, such as erythromycin. The N-terminal subdomain, an interdomain linker, is a truncated Rossmann fold which acts to stabilizes the catalytic subdomain. Unlike typical SDRs, the isolated domain does not oligomerize but is composed of 2 subdomains, each resembling an SDR monomer. The active site resembles that of typical SDRs, except that the usual positions of the catalytic Asn and Tyr are swapped, so that the canonical YXXXK motif changes to YXXXN. Modular PKSs are multifunctional structures in which the makeup recapitulates that found in (and may have evolved from) FAS. Polyketide synthesis also proceeds via the addition of 2-carbon units as in fatty acid synthesis. The complex SDR NADP-binding motif, GGXGXXG, is often present, but is not strictly conserved in each instance of the module. This subfamily includes both KR domains of the Bacillus subtilis Pks J,-L, and PksM, and all three KR domains of PksN, components of the megacomplex bacillaene synthase, which synthesizes the antibiotic bacillaene. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold (alpha/beta folding pattern with a central beta-sheet), an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Classical SDRs are typically about 250 residues long, while extended SDRs are approximately 350 residues. Sequence identity between different SDR enzymes are typically in the 15-30% range, but the enzymes share the Rossmann fold NAD-binding motif and characteristic NAD-binding and catalytic sequence patterns. These enzymes catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human prostaglandin dehydrogenase (PGDH) numbering). In addition to the Tyr and Lys, there is often an upstream Ser (Ser-138, PGDH numbering) and/or an Asn (Asn-107, PGDH numbering) contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Extended SDRs have additional elements in the C-terminal region, and typically have a TGXXGXXG cofactor binding motif. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type KRs have a TGXXXGX(1-2)G NAD(P)-binding motif. Some atypical SDRs have lost catalytic activity and/or have an unusual NAD(P)-binding motif and missing or unusual active site residues. Reactions catalyzed within the SDR family include isomerization, decarboxylation, epimerization, C=N bond reduction, dehydratase activity, dehalogenation, Enoyl-CoA reduction, and carbonyl-alcohol oxidoreduction.


Pssm-ID: 187656 [Multi-domain]  Cd Length: 436  Bit Score: 53.14  E-value: 1.64e-08
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  11 VYLVTGGCGFLGEHVVRMLLQREPRlgelRVF----------DQHLGPWLEELKTGPVRVTAIQGDVTQAHEVAAAVAGA 80
Cdd:cd08953   207 VYLVTGGAGGIGRALARALARRYGA----RLVllgrsplppeEEWKAQTLAALEALGARVLYISADVTDAAAVRRLLEKV 282
                          90       100       110       120       130       140
                  ....*....|....*....|....*....|....*....|....*....|....*....|..
gi 1034596152  81 HVV-------IHTAGLVDV--FGRASPKTIHEV---NVQGTRNVIEACVQTGTRFLVYTSSM 130
Cdd:cd08953   283 RERygaidgvIHAAGVLRDalLAQKTAEDFEAVlapKVDGLLNLAQALADEPLDFFVLFSSV 344
SDR_e_a cd05226
Extended (e) and atypical (a) SDRs; Extended or atypical short-chain dehydrogenases/reductases ...
13-176 1.86e-08

Extended (e) and atypical (a) SDRs; Extended or atypical short-chain dehydrogenases/reductases (SDRs, aka tyrosine-dependent oxidoreductases) are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Atypical SDRs include biliverdin IX beta reductase (BVR-B,aka flavin reductase), NMRa (a negative transcriptional regulator of various fungi), progesterone 5-beta-reductase like proteins, phenylcoumaran benzylic ether and pinoresinol-lariciresinol reductases, phenylpropene synthases, eugenol synthase, triphenylmethane reductase, isoflavone reductases, and others. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187537 [Multi-domain]  Cd Length: 176  Bit Score: 51.63  E-value: 1.86e-08
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQReprlG-ELRVFDQH-LGPWLEELKtgpvRVTAIQGDVTQAHEVAAAVAGAHVVIHTAGLv 90
Cdd:cd05226     2 LILGATGFIGRALARELLEQ----GhEVTLLVRNtKRLSKEDQE----PVAVVEGDLRDLDSLSDAVQGVDVVIHLAGA- 72
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  91 DVFGRAspktIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTkghpfyrgnEDTPYEAvhRHPYPCSKALAEWLV 170
Cdd:cd05226    73 PRDTRD----FCEVDVEGTRNVLEAAKEAGVKHFIFISSLGAYGDLH---------EETEPSP--SSPYLAVKAKTEAVL 137

                  ....*.
gi 1034596152 171 LEANGR 176
Cdd:cd05226   138 REASLP 143
UDP_G4E_1_SDR_e cd05247
UDP-glucose 4 epimerase, subgroup 1, extended (e) SDRs; UDP-glucose 4 epimerase (aka ...
12-169 5.27e-08

UDP-glucose 4 epimerase, subgroup 1, extended (e) SDRs; UDP-glucose 4 epimerase (aka UDP-galactose-4-epimerase), is a homodimeric extended SDR. It catalyzes the NAD-dependent conversion of UDP-galactose to UDP-glucose, the final step in Leloir galactose synthesis. This subgroup has the characteristic active site tetrad and NAD-binding motif of the extended SDRs. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187558 [Multi-domain]  Cd Length: 323  Bit Score: 51.77  E-value: 5.27e-08
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQReprlG-ELRVFD-------QHLgPWLEelktgPVRVTAIQGDV--TQAHEVAAAVAGAH 81
Cdd:cd05247     2 VLVTGGAGYIGSHTVVELLEA----GyDVVVLDnlsnghrEAL-PRIE-----KIRIEFYEGDIrdRAALDKVFAEHKID 71
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  82 VVIHTAGLVDVfGR--ASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKGhPFYrgnEDTPYEAVhrHPY 159
Cdd:cd05247    72 AVIHFAALKAV-GEsvQKPLKYYDNNVVGTLNLLEAMRAHGVKNFVFSSSAAVYGEPETV-PIT---EEAPLNPT--NPY 144
                         170
                  ....*....|
gi 1034596152 160 PCSKALAEWL 169
Cdd:cd05247   145 GRTKLMVEQI 154
RfbD COG1091
dTDP-4-dehydrorhamnose reductase [Cell wall/membrane/envelope biogenesis];
13-176 1.36e-07

dTDP-4-dehydrorhamnose reductase [Cell wall/membrane/envelope biogenesis];


Pssm-ID: 440708 [Multi-domain]  Cd Length: 279  Bit Score: 50.13  E-value: 1.36e-07
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREPRL-----GELRVFDqhlgpwLEELKTgpvRVTAIQGDVTqahevaaavagahvvIHTA 87
Cdd:COG1091     3 LVTGANGQLGRALVRLLAERGYEVvaldrSELDITD------PEAVAA---LLEEVRPDVV---------------INAA 58
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  88 GLVDVFGRAS-PKTIHEVNVQGTRNVIEACVQTGTRfLVYTSSMEVvgpntkghpfYRGNEDTPY-EAVHRHP---YPCS 162
Cdd:COG1091    59 AYTAVDKAESePELAYAVNATGPANLAEACAELGAR-LIHISTDYV----------FDGTKGTPYtEDDPPNPlnvYGRS 127
                         170
                  ....*....|....
gi 1034596152 163 KALAEWLVLEANGR 176
Cdd:COG1091   128 KLAGEQAVRAAGPR 141
GDP_MD_SDR_e cd05260
GDP-mannose 4,6 dehydratase, extended (e) SDRs; GDP-mannose 4,6 dehydratase, a homodimeric SDR, ...
13-179 2.28e-07

GDP-mannose 4,6 dehydratase, extended (e) SDRs; GDP-mannose 4,6 dehydratase, a homodimeric SDR, catalyzes the NADP(H)-dependent conversion of GDP-(D)-mannose to GDP-4-keto, 6-deoxy-(D)-mannose in the fucose biosynthesis pathway. These proteins have the canonical active site triad and NAD-binding pattern, however the active site Asn is often missing and may be substituted with Asp. A Glu residue has been identified as an important active site base. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187570 [Multi-domain]  Cd Length: 316  Bit Score: 49.90  E-value: 2.28e-07
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREPRL-GELRVFDQHLGPWLEELKTGPVRVTAIQGDVTQahevaaavagahvvihTAGLVD 91
Cdd:cd05260     3 LITGITGQDGSYLAEFLLEKGYEVhGIVRRSSSFNTDRIDHLYINKDRITLHYGDLTD----------------SSSLRR 66
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  92 VFGRASPKTI-H------------------EVNVQGTRNVIEACVQTG--TRFLVYTSSmEVVGPNTKgHPFyrgNEDTP 150
Cdd:cd05260    67 AIEKVRPDEIyHlaaqshvkvsfddpeytaEVNAVGTLNLLEAIRILGldARFYQASSS-EEYGKVQE-LPQ---SETTP 141
                         170       180       190
                  ....*....|....*....|....*....|..
gi 1034596152 151 YEAvhRHPYPCSKALAEWLVL---EANGRKAM 179
Cdd:cd05260   142 FRP--RSPYAVSKLYADWITRnyrEAYGLFAV 171
UDP_G4E_5_SDR_e cd05264
UDP-glucose 4-epimerase (G4E), subgroup 5, extended (e) SDRs; This subgroup partially ...
12-129 2.61e-07

UDP-glucose 4-epimerase (G4E), subgroup 5, extended (e) SDRs; This subgroup partially conserves the characteristic active site tetrad and NAD-binding motif of the extended SDRs, and has been identified as possible UDP-glucose 4-epimerase (aka UDP-galactose 4-epimerase), a homodimeric member of the extended SDR family. UDP-glucose 4-epimerase catalyzes the NAD-dependent conversion of UDP-galactose to UDP-glucose, the final step in Leloir galactose synthesis. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187574 [Multi-domain]  Cd Length: 300  Bit Score: 49.62  E-value: 2.61e-07
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREPRlgeLRVFDQHLGPwlEELKTGPVRVtaIQGDVTQAHEVAAAVAGAHVVIHTAGlvD 91
Cdd:cd05264     2 VLIVGGNGFIGSHLVDALLEEGPQ---VRVFDRSIPP--YELPLGGVDY--IKGDYENRADLESALVGIDTVIHLAS--T 72
                          90       100       110       120
                  ....*....|....*....|....*....|....*....|.
gi 1034596152  92 VFGRASPKTIH---EVNVQGTRNVIEACVQTGTRFLVYTSS 129
Cdd:cd05264    73 TNPATSNKNPIldiQTNVAPTVQLLEACAAAGIGKIIFASS 113
YbjT COG0702
Uncharacterized conserved protein YbjT, contains NAD(P)-binding and DUF2867 domains [General ...
12-130 2.68e-07

Uncharacterized conserved protein YbjT, contains NAD(P)-binding and DUF2867 domains [General function prediction only];


Pssm-ID: 440466 [Multi-domain]  Cd Length: 215  Bit Score: 49.07  E-value: 2.68e-07
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREprlGELRVFDQHLGPWLEELKTGpvrVTAIQGDVTQAhevaaavagahvvihtAGLVD 91
Cdd:COG0702     2 ILVTGATGFIGRRVVRALLARG---HPVRALVRDPEKAAALAAAG---VEVVQGDLDDP----------------ESLAA 59
                          90       100       110       120
                  ....*....|....*....|....*....|....*....|....*...
gi 1034596152  92 VFGRA---------SPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSM 130
Cdd:COG0702    60 ALAGVdavfllvpsGPGGDFAVDVEGARNLADAAKAAGVKRIVYLSAL 107
PKS_KR smart00822
This enzymatic domain is part of bacterial polyketide synthases; It catalyses the first step ...
11-130 2.74e-07

This enzymatic domain is part of bacterial polyketide synthases; It catalyses the first step in the reductive modification of the beta-carbonyl centres in the growing polyketide chain. It uses NADPH to reduce the keto group to a hydroxy group.


Pssm-ID: 214833 [Multi-domain]  Cd Length: 180  Bit Score: 48.63  E-value: 2.74e-07
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152   11 VYLVTGGCGFLGEHVVRMLLQREPRlgelrvfdqHL------GP-------WLEELKTGPVRVTAIQGDVTQAHEVAAAV 77
Cdd:smart00822   2 TYLITGGLGGLGRALARWLAERGAR---------RLvllsrsGPdapgaaaLLAELEAAGARVTVVACDVADRDALAAVL 72
                           90       100       110       120       130       140
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*
gi 1034596152   78 AGAHVV-------IHTAGLVD--VFGRASPKTIHEVN---VQGTRNVIEACVQTGTRFLVYTSSM 130
Cdd:smart00822  73 AAIPAVegpltgvIHAAGVLDdgVLASLTPERFAAVLapkAAGAWNLHELTADLPLDFFVLFSSI 137
dTDP_HR_like_SDR_e cd05254
dTDP-6-deoxy-L-lyxo-4-hexulose reductase and related proteins, extended (e) SDRs; ...
13-176 1.74e-06

dTDP-6-deoxy-L-lyxo-4-hexulose reductase and related proteins, extended (e) SDRs; dTDP-6-deoxy-L-lyxo-4-hexulose reductase, an extended SDR, synthesizes dTDP-L-rhamnose from alpha-D-glucose-1-phosphate, providing the precursor of L-rhamnose, an essential cell wall component of many pathogenic bacteria. This subgroup has the characteristic active site tetrad and NADP-binding motif. This subgroup also contains human MAT2B, the regulatory subunit of methionine adenosyltransferase (MAT); MAT catalyzes S-adenosylmethionine synthesis. The human gene encoding MAT2B encodes two major splicing variants which are induced in human cell liver cancer and regulate HuR, an mRNA-binding protein which stabilizes the mRNA of several cyclins, to affect cell proliferation. Both MAT2B variants include this extended SDR domain. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187564 [Multi-domain]  Cd Length: 280  Bit Score: 46.85  E-value: 1.74e-06
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQR------------EPRLGELRVFDQhlgpwLEELktgpvrVTAIQGDVtqahevaaavaga 80
Cdd:cd05254     3 LITGATGMLGRALVRLLKERgyevigtgrsraSLFKLDLTDPDA-----VEEA------IRDYKPDV------------- 58
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  81 hvVIHTAGLVDVFGRAS-PKTIHEVNVQGTRNVIEACVQTGTRfLVYTSSmEVVGPNTKghPFYRgNEDTPyeavhrHP- 158
Cdd:cd05254    59 --IINCAAYTRVDKCESdPELAYRVNVLAPENLARAAKEVGAR-LIHIST-DYVFDGKK--GPYK-EEDAP------NPl 125
                         170       180
                  ....*....|....*....|
gi 1034596152 159 --YPCSKALAEWLVLEANGR 176
Cdd:cd05254   126 nvYGKSKLLGEVAVLNANPR 145
KR pfam08659
KR domain; This enzymatic domain is part of bacterial polyketide synthases and catalyzes the ...
11-130 4.59e-06

KR domain; This enzymatic domain is part of bacterial polyketide synthases and catalyzes the first step in the reductive modification of the beta-carbonyl centres in the growing polyketide chain. It uses NADPH to reduce the keto group to a hydroxy group.


Pssm-ID: 430138 [Multi-domain]  Cd Length: 180  Bit Score: 44.86  E-value: 4.59e-06
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  11 VYLVTGGCGFLGEHVVRMLLQREPRlgELRVFDQHLGP------WLEELKTGPVRVTAIQGDVTQAHEVAAAVAGAHVV- 83
Cdd:pfam08659   2 TYLITGGLGGLGRELARWLAERGAR--HLVLLSRSAAPrpdaqaLIAELEARGVEVVVVACDVSDPDAVAALLAEIKAEg 79
                          90       100       110       120       130
                  ....*....|....*....|....*....|....*....|....*....|....*...
gi 1034596152  84 ------IHTAGLVD--VFGRASPKTIHEVN---VQGTRNVIEACVQTGTRFLVYTSSM 130
Cdd:pfam08659  80 ppirgvIHAAGVLRdaLLENMTDEDWRRVLapkVTGTWNLHEATPDEPLDFFVLFSSI 137
UDP_GE_SDE_e cd05253
UDP glucuronic acid epimerase, extended (e) SDRs; This subgroup contains UDP-D-glucuronic acid ...
12-142 6.42e-06

UDP glucuronic acid epimerase, extended (e) SDRs; This subgroup contains UDP-D-glucuronic acid 4-epimerase, an extended SDR, which catalyzes the conversion of UDP-alpha-D-glucuronic acid to UDP-alpha-D-galacturonic acid. This group has the SDR's canonical catalytic tetrad and the TGxxGxxG NAD-binding motif of the extended SDRs. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187563 [Multi-domain]  Cd Length: 332  Bit Score: 45.40  E-value: 6.42e-06
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQR--------------EPRLGELRvfdqhlgpwLEELKTgPVRVTAIQGDVT--QAHEVAA 75
Cdd:cd05253     3 ILVTGAAGFIGFHVAKRLLERgdevvgidnlndyyDVRLKEAR---------LELLGK-SGGFKFVKGDLEdrEALRRLF 72
                          90       100       110       120       130       140       150
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  76 AVAGAHVVIHTAGLVDVfgRAS---PKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTKgHPF 142
Cdd:cd05253    73 KDHEFDAVIHLAAQAGV--RYSlenPHAYVDSNIVGFLNLLELCRHFGVKHLVYASSSSVYGLNTK-MPF 139
UGD_SDR_e cd05230
UDP-glucuronate decarboxylase (UGD) and related proteins, extended (e) SDRs; UGD catalyzes the ...
13-172 9.71e-06

UDP-glucuronate decarboxylase (UGD) and related proteins, extended (e) SDRs; UGD catalyzes the formation of UDP-xylose from UDP-glucuronate; it is an extended-SDR, and has the characteristic glycine-rich NAD-binding pattern, TGXXGXXG, and active site tetrad. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187541 [Multi-domain]  Cd Length: 305  Bit Score: 44.94  E-value: 9.71e-06
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLqrepRLG-ELRVFDQHL-GPW--LEELKTGPvRVTAIQGDVTQahevaAAVAGAHVVIHTAg 88
Cdd:cd05230     4 LITGGAGFLGSHLCDRLL----EDGhEVICVDNFFtGRKrnIEHLIGHP-NFEFIRHDVTE-----PLYLEVDQIYHLA- 72
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  89 lvdvfGRASP--------KTIhEVNVQGTRNVIEACVQTGTRFLvYTSSMEVVGpNTKGHP---FYRGNEDT--Pyeavh 155
Cdd:cd05230    73 -----CPASPvhyqynpiKTL-KTNVLGTLNMLGLAKRVGARVL-LASTSEVYG-DPEVHPqpeSYWGNVNPigP----- 139
                         170
                  ....*....|....*..
gi 1034596152 156 RHPYPCSKALAEWLVLE 172
Cdd:cd05230   140 RSCYDEGKRVAETLCMA 156
PLN02686 PLN02686
cinnamoyl-CoA reductase
2-130 1.20e-05

cinnamoyl-CoA reductase


Pssm-ID: 215370  Cd Length: 367  Bit Score: 44.77  E-value: 1.20e-05
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152   2 ADSAQAQKLVyLVTGGCGFLGEHVVRMLLQR-------------EPRLGELRVFDqhlgpwleELKTGPVRVTAIQGDVT 68
Cdd:PLN02686   47 AGADAEARLV-CVTGGVSFLGLAIVDRLLRHgysvriavdtqedKEKLREMEMFG--------EMGRSNDGIWTVMANLT 117
                          90       100       110       120       130       140
                  ....*....|....*....|....*....|....*....|....*....|....*....|....
gi 1034596152  69 QAHEVAAAVAGAHVVIHTAGLVDVFGRAS-PKTIHEVNVQGTRNVIEACVQTGT-RFLVYTSSM 130
Cdd:PLN02686  118 EPESLHEAFDGCAGVFHTSAFVDPAGLSGyTKSMAELEAKASENVIEACVRTESvRKCVFTSSL 181
UDP_invert_4-6DH_SDR_e cd05237
UDP-Glcnac (UDP-linked N-acetylglucosamine) inverting 4,6-dehydratase, extended (e) SDRs; ...
13-177 1.29e-04

UDP-Glcnac (UDP-linked N-acetylglucosamine) inverting 4,6-dehydratase, extended (e) SDRs; UDP-Glcnac inverting 4,6-dehydratase was identified in Helicobacter pylori as the hexameric flaA1 gene product (FlaA1). FlaA1 is hexameric, possesses UDP-GlcNAc-inverting 4,6-dehydratase activity, and catalyzes the first step in the creation of a pseudaminic acid derivative in protein glycosylation. Although this subgroup has the NADP-binding motif characteristic of extended SDRs, its members tend to have a Met substituted for the active site Tyr found in most SDR families. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187548 [Multi-domain]  Cd Length: 287  Bit Score: 41.45  E-value: 1.29e-04
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREPRlgELRVFD-----QH-LGPWLEELKTGPVRVTAIqGDV--TQAHEVAAAVAGAHVVI 84
Cdd:cd05237     6 LVTGGAGSIGSELVRQILKFGPK--KLIVFDrdenkLHeLVRELRSRFPHDKLRFII-GDVrdKERLRRAFKERGPDIVF 82
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  85 HTAGLVDVfgRA---SPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGP-NTKGhpfyrgnedtpyeavhrhpyp 160
Cdd:cd05237    83 HAAALKHV--PSmedNPEEAIKTNVLGTKNVIDAAIENGVEKFVCISTDKAVNPvNVMG--------------------- 139
                         170
                  ....*....|....*..
gi 1034596152 161 CSKALAEWLVLEANGRK 177
Cdd:cd05237   140 ATKRVAEKLLLAKNEYS 156
FAR-N_SDR_e cd05236
fatty acyl CoA reductases (FARs), extended (e) SDRs; SDRs are Rossmann-fold NAD(P)H-binding ...
12-172 2.14e-04

fatty acyl CoA reductases (FARs), extended (e) SDRs; SDRs are Rossmann-fold NAD(P)H-binding proteins, many of which may function as fatty acyl CoA reductases (FAR), acting on medium and long chain fatty acids, and have been reported to be involved in diverse processes such as biosynthesis of insect pheromones, plant cuticular wax production, and mammalian wax biosynthesis. In Arabidopsis thaliana, proteins with this particular architecture have also been identified as the MALE STERILITY 2 (MS2) gene product, which is implicated in male gametogenesis. Mutations in MS2 inhibit the synthesis of exine (sporopollenin), rendering plants unable to reduce pollen wall fatty acids to corresponding alcohols. This N-terminal domain shares the catalytic triad (but not the upstream Asn) and characteristic NADP-binding motif of the extended SDR family. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187547 [Multi-domain]  Cd Length: 320  Bit Score: 41.13  E-value: 2.14e-04
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREPRLGELRVF----DQHLG-PWLEELKTGPV-------------RVTAIQGDVTQ---- 69
Cdd:cd05236     3 VLITGATGFLGKVLLEKLLRSCPDIGKIYLLirgkSGQSAeERLRELLKDKLfdrgrnlnplfesKIVPIEGDLSEpnlg 82
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  70 --AHEVAAAVAGAHVVIHTAGLVDvFGRASPKTIhEVNVQGTRNVIEACVQ-TGTRFLVYTSS----------MEVVGP- 135
Cdd:cd05236    83 lsDEDLQTLIEEVNIIIHCAATVT-FDERLDEAL-SINVLGTLRLLELAKRcKKLKAFVHVSTayvngdrqliEEKVYPp 160
                         170       180       190       200
                  ....*....|....*....|....*....|....*....|....*..
gi 1034596152 136 --NTKGHPFYR------GNEDTPYEAVHRHP--YPCSKALAEWLVLE 172
Cdd:cd05236   161 paDPEKLIDILelmddlELERATPKLLGGHPntYTFTKALAERLVLK 207
WbmH_like_SDR_e cd08957
Bordetella bronchiseptica enzymes WbmH and WbmG-like, extended (e) SDRs; Bordetella ...
13-126 5.25e-04

Bordetella bronchiseptica enzymes WbmH and WbmG-like, extended (e) SDRs; Bordetella bronchiseptica enzymes WbmH and WbmG, and related proteins. This subgroup exhibits the active site tetrad and NAD-binding motif of the extended SDR family. It has been proposed that the active site in Bordetella WbmG and WbmH cannot function as an epimerase, and that it plays a role in O-antigen synthesis pathway from UDP-2,3-diacetamido-2,3-dideoxy-l-galacturonic acid. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187660 [Multi-domain]  Cd Length: 307  Bit Score: 39.79  E-value: 5.25e-04
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLqrePRLGELRVFDQHLGPWLEELKTGPvRVTAIQGDVTQahevaaavagahvvihtAGLVD- 91
Cdd:cd08957     4 LITGGAGQIGSHLIEHLL---ERGHQVVVIDNFATGRREHLPDHP-NLTVVEGSIAD-----------------KALVDk 62
                          90       100       110       120       130
                  ....*....|....*....|....*....|....*....|....*....|.
gi 1034596152  92 VFGRASP-KTIH---------------EVNVQGTRNVIEACVQTGTRFLVY 126
Cdd:cd08957    63 LFGDFKPdAVVHtaaaykdpddwyedtLTNVVGGANVVQAAKKAGVKRLIY 113
PLN02166 PLN02166
dTDP-glucose 4,6-dehydratase
8-172 8.16e-04

dTDP-glucose 4,6-dehydratase


Pssm-ID: 165812 [Multi-domain]  Cd Length: 436  Bit Score: 39.22  E-value: 8.16e-04
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152   8 QKLVYLVTGGCGFLGEHVVRMLLQREprlGELRVFDQHLGPWLEELKT--GPVRVTAIQGDVTQahevaaavagaHVVIH 85
Cdd:PLN02166  119 KRLRIVVTGGAGFVGSHLVDKLIGRG---DEVIVIDNFFTGRKENLVHlfGNPRFELIRHDVVE-----------PILLE 184
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  86 TAGLVDVFGRASP--------KTIhEVNVQGTRNVIEACVQTGTRFLVyTSSMEVVGPNTKgHP---FYRGNEDTPYEav 154
Cdd:PLN02166  185 VDQIYHLACPASPvhykynpvKTI-KTNVMGTLNMLGLAKRVGARFLL-TSTSEVYGDPLE-HPqkeTYWGNVNPIGE-- 259
                         170
                  ....*....|....*...
gi 1034596152 155 hRHPYPCSKALAEWLVLE 172
Cdd:PLN02166  260 -RSCYDEGKRTAETLAMD 276
SDR_a5 cd05243
atypical (a) SDRs, subgroup 5; This subgroup contains atypical SDRs, some of which are ...
13-167 1.29e-03

atypical (a) SDRs, subgroup 5; This subgroup contains atypical SDRs, some of which are identified as putative NAD(P)-dependent epimerases, one as a putative NAD-dependent epimerase/dehydratase. Atypical SDRs are distinct from classical SDRs. Members of this subgroup have a glycine-rich NAD(P)-binding motif that is very similar to the extended SDRs, GXXGXXG, and binds NADP. Generally, this subgroup has poor conservation of the active site tetrad; however, individual sequences do contain matches to the YXXXK active site motif, the upstream Ser, and there is a highly conserved Asp in place of the usual active site Asn throughout the subgroup. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Atypical SDRs include biliverdin IX beta reductase (BVR-B,aka flavin reductase), NMRa (a negative transcriptional regulator of various fungi), progesterone 5-beta-reductase like proteins, phenylcoumaran benzylic ether and pinoresinol-lariciresinol reductases, phenylpropene synthases, eugenol synthase, triphenylmethane reductase, isoflavone reductases, and others. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. In addition to the Rossmann fold core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids, and typically have a TGXXGXXG cofactor binding motif. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187554 [Multi-domain]  Cd Length: 203  Bit Score: 38.37  E-value: 1.29e-03
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQR--EPRLGeLRVFDQhlgpwLEELKtgPVRVTAIQGDVTQAHEVAAAVAGAHVVIHTAGLv 90
Cdd:cd05243     3 LVVGATGKVGRHVVRELLDRgyQVRAL-VRDPSQ-----AEKLE--AAGAEVVVGDLTDAESLAAALEGIDAVISAAGS- 73
                          90       100       110       120       130       140       150
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1034596152  91 dvfGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMevvgpntkghpfyrGNEDTPYEAVHRHPYPCSKALAE 167
Cdd:cd05243    74 ---GGKGGPRTEAVDYDGNINLIDAAKKAGVKRFVLVSSI--------------GADKPSHPLEALGPYLDAKRKAE 133
TDH_SDR_e cd05272
L-threonine dehydrogenase, extended (e) SDRs; This subgroup contains members identified as ...
84-169 1.54e-03

L-threonine dehydrogenase, extended (e) SDRs; This subgroup contains members identified as L-threonine dehydrogenase (TDH). TDH catalyzes the zinc-dependent formation of 2-amino-3-ketobutyrate from L-threonine via NAD(H)-dependent oxidation. This group is distinct from TDHs that are members of the medium chain dehydrogenase/reductase family. This group has the NAD-binding motif and active site tetrad of the extended SDRs. Extended SDRs are distinct from classical SDRs. In addition to the Rossmann fold (alpha/beta folding pattern with a central beta-sheet) core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids. Extended SDRs are a diverse collection of proteins, and include isomerases, epimerases, oxidoreductases, and lyases; they typically have a TGXXGXXG cofactor binding motif. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. Atypical SDRs generally lack the catalytic residues characteristic of the SDRs, and their glycine-rich NAD(P)-binding motif is often different from the forms normally seen in classical or extended SDRs. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187580 [Multi-domain]  Cd Length: 308  Bit Score: 38.45  E-value: 1.54e-03
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  84 IHTAGLVDVFGRASPKTIHEVNVQGTRNVIEACVQTGTRFLVyTSSMEVVGPNTkghpfyrGNEDTPYEAVHRhP---YP 160
Cdd:cd05272    70 IHLAALLSAVGEKNPPLAWDVNMNGLHNVLELAREHNLRIFV-PSTIGAFGPTT-------PRNNTPDDTIQR-PrtiYG 140

                  ....*....
gi 1034596152 161 CSKALAEWL 169
Cdd:cd05272   141 VSKVAAELL 149
PLN02214 PLN02214
cinnamoyl-CoA reductase
14-133 4.46e-03

cinnamoyl-CoA reductase


Pssm-ID: 177862 [Multi-domain]  Cd Length: 342  Bit Score: 37.04  E-value: 4.46e-03
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  14 VTGGCGFLGEHVVRMLLQREPRL-GELRVFDQHLGPWLEELKTGPVRVTAIQGDVTQAHEVAAAVAGAHVVIHTAGLVDv 92
Cdd:PLN02214   15 VTGAGGYIASWIVKILLERGYTVkGTVRNPDDPKNTHLRELEGGKERLILCKADLQDYEALKAAIDGCDGVFHTASPVT- 93
                          90       100       110       120
                  ....*....|....*....|....*....|....*....|.
gi 1034596152  93 fgrASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVV 133
Cdd:PLN02214   94 ---DDPEQMVEPAVNGAKFVINAAAEAKVKRVVITSSIGAV 131
PRK10675 PRK10675
UDP-galactose-4-epimerase; Provisional
13-151 4.59e-03

UDP-galactose-4-epimerase; Provisional


Pssm-ID: 182639 [Multi-domain]  Cd Length: 338  Bit Score: 37.10  E-value: 4.59e-03
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQ--REPR-LGELRVFDQHLGPWLEELktGPVRVTAIQGDVTQAHEVAA--AVAGAHVVIHTA 87
Cdd:PRK10675    4 LVTGGSGYIGSHTCVQLLQngHDVViLDNLCNSKRSVLPVIERL--GGKHPTFVEGDIRNEALLTEilHDHAIDTVIHFA 81
                          90       100       110       120       130       140
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....
gi 1034596152  88 GLVDVfGR--ASPKTIHEVNVQGTRNVIEACVQTGTRFLVYTSSMEVVGPNTK---GHPFYRGNEDTPY 151
Cdd:PRK10675   82 GLKAV-GEsvQKPLEYYDNNVNGTLRLISAMRAANVKNLIFSSSATVYGDQPKipyVESFPTGTPQSPY 149
TMR_SDR_a cd05269
triphenylmethane reductase (TMR)-like proteins, NMRa-like, atypical (a) SDRs; TMR is an ...
12-128 6.92e-03

triphenylmethane reductase (TMR)-like proteins, NMRa-like, atypical (a) SDRs; TMR is an atypical NADP-binding protein of the SDR family. It lacks the active site residues of the SDRs but has a glycine rich NAD(P)-binding motif that matches the extended SDRs. Proteins in this subgroup however, are more similar in length to the classical SDRs. TMR was identified as a reducer of triphenylmethane dyes, important environmental pollutants. This subgroup also includes Escherichia coli NADPH-dependent quinine oxidoreductase (QOR2), which catalyzes two-electron reduction of quinone; but is unlikely to play a major role in protecting against quinone cytotoxicity. Atypical SDRs are distinct from classical SDRs. Atypical SDRs include biliverdin IX beta reductase (BVR-B,aka flavin reductase), NMRa (a negative transcriptional regulator of various fungi), progesterone 5-beta-reductase like proteins, phenylcoumaran benzylic ether and pinoresinol-lariciresinol reductases, phenylpropene synthases, eugenol synthase, triphenylmethane reductase, isoflavone reductases, and others. SDRs are a functionally diverse family of oxidoreductases that have a single domain with a structurally conserved Rossmann fold, an NAD(P)(H)-binding region, and a structurally diverse C-terminal region. Sequence identity between different SDR enzymes is typically in the 15-30% range; they catalyze a wide range of activities including the metabolism of steroids, cofactors, carbohydrates, lipids, aromatic compounds, and amino acids, and act in redox sensing. Classical SDRs have an TGXXX[AG]XG cofactor binding motif and a YXXXK active site motif, with the Tyr residue of the active site motif serving as a critical catalytic residue (Tyr-151, human 15-hydroxyprostaglandin dehydrogenase numbering). In addition to the Tyr and Lys, there is often an upstream Ser and/or an Asn, contributing to the active site; while substrate binding is in the C-terminal region, which determines specificity. The standard reaction mechanism is a 4-pro-S hydride transfer and proton relay involving the conserved Tyr and Lys, a water molecule stabilized by Asn, and nicotinamide. In addition to the Rossmann fold core region typical of all SDRs, extended SDRs have a less conserved C-terminal extension of approximately 100 amino acids, and typically have a TGXXGXXG cofactor binding motif. Complex (multidomain) SDRs such as ketoreductase domains of fatty acid synthase have a GGXGXXG NAD(P)-binding motif and an altered active site motif (YXXXN). Fungal type ketoacyl reductases have a TGXXXGX(1-2)G NAD(P)-binding motif.


Pssm-ID: 187578 [Multi-domain]  Cd Length: 272  Bit Score: 36.48  E-value: 6.92e-03
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  12 YLVTGGCGFLGEHVVRMLLQREPRLGEL-RVFDQhlgpwLEELKTGPVRVTaiQGDVTQAhevaaavagahvvihtAGLV 90
Cdd:cd05269     1 ILVTGATGKLGTAVVELLLAKVASVVALvRNPEK-----AKAFAADGVEVR--QGDYDDP----------------ETLE 57
                          90       100       110       120
                  ....*....|....*....|....*....|....*....|....
gi 1034596152  91 DVF---GRA---SPkTIHEVNVQGTRNVIEACVQTGTRFLVYTS 128
Cdd:cd05269    58 RAFegvDRLlliSP-SDLEDRIQQHKNFIDAAKQAGVKHIVYLS 100
RmlD_sub_bind pfam04321
RmlD substrate binding domain; L-rhamnose is a saccharide required for the virulence of some ...
13-176 7.69e-03

RmlD substrate binding domain; L-rhamnose is a saccharide required for the virulence of some bacteria. Its precursor, dTDP-L-rhamnose, is synthesized by four different enzymes the final one of which is RmlD. The RmlD substrate binding domain is responsible for binding a sugar nucleotide.


Pssm-ID: 427865 [Multi-domain]  Cd Length: 284  Bit Score: 36.10  E-value: 7.69e-03
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  13 LVTGGCGFLGEHVVRMLLQREPRLgelrvfdqhLGPWLEELK-TGPVRVT----AIQGDVTqahevaaavagahvvIHTA 87
Cdd:pfam04321   2 LITGANGQLGTELRRLLAERGIEV---------VALTRAELDlTDPEAVArllrEIKPDVV---------------VNAA 57
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  88 GLVDVFGRAS-PKTIHEVNVQGTRNVIEACVQTGTrFLVYTSSMEVvgpntkghpfYRGNEDTPYEAVHR-HP---YPCS 162
Cdd:pfam04321  58 AYTAVDKAESePDLAYAINALAPANLAEACAAVGA-PLIHISTDYV----------FDGTKPRPYEEDDEtNPlnvYGRT 126
                         170
                  ....*....|....
gi 1034596152 163 KALAEWLVLEANGR 176
Cdd:pfam04321 127 KLAGEQAVRAAGPR 140
PLN02896 PLN02896
cinnamyl-alcohol dehydrogenase
6-130 8.29e-03

cinnamyl-alcohol dehydrogenase


Pssm-ID: 178484 [Multi-domain]  Cd Length: 353  Bit Score: 36.34  E-value: 8.29e-03
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152   6 QAQKLVYLVTGGCGFLGEHVVRMLLQREPRL-GELRVFD--QHLGPWLEELKtgpvRVTAIQGDVTQAHEVAAAVAGAHV 82
Cdd:PLN02896    7 ESATGTYCVTGATGYIGSWLVKLLLQRGYTVhATLRDPAksLHLLSKWKEGD----RLRLFRADLQEEGSFDEAVKGCDG 82
                          90       100       110       120       130
                  ....*....|....*....|....*....|....*....|....*....|....*...
gi 1034596152  83 VIHTAGLVDvFGRASPKTIHEVNVQ---------GTRNVIEACVQTGT-RFLVYTSSM 130
Cdd:PLN02896   83 VFHVAASME-FDVSSDHNNIEEYVQskvidpaikGTLNVLKSCLKSKTvKRVVFTSSI 139
PLN00198 PLN00198
anthocyanidin reductase; Provisional
1-174 9.20e-03

anthocyanidin reductase; Provisional


Pssm-ID: 215100 [Multi-domain]  Cd Length: 338  Bit Score: 36.02  E-value: 9.20e-03
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152   1 MADSAQAQKLVYLVTGGCGFLGEHVVRMLLQ---------REP----RLGELRVFdQHLGpwleELKTgpvrvtaIQGDV 67
Cdd:PLN00198    1 MATLTPTGKKTACVIGGTGFLASLLIKLLLQkgyavnttvRDPenqkKIAHLRAL-QELG----DLKI-------FGADL 68
                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1034596152  68 TQAHEVAAAVAGAHVVIHTAGLVDVFGRASPKTIHEVNVQGTRNVIEACVQTGT-RFLVYTSSMEVVGPNTKGHPFYRGN 146
Cdd:PLN00198   69 TDEESFEAPIAGCDLVFHVATPVNFASEDPENDMIKPAIQGVHNVLKACAKAKSvKRVILTSSAAAVSINKLSGTGLVMN 148
                         170       180       190
                  ....*....|....*....|....*....|....*...
gi 1034596152 147 E----DTPYEAVHRHP---YPCSKALAE---WLVLEAN 174
Cdd:PLN00198  149 EknwtDVEFLTSEKPPtwgYPASKTLAEkaaWKFAEEN 186
 
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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