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Conserved domains on  [gi|2633308|emb|CAB12812|]
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putative NADH-flavin oxidoreductase [Bacillus subtilis subsp. subtilis str. 168]

Protein Classification

SDR family oxidoreductase( domain architecture ID 10142826)

atypical SDR (short-chain dehydrogenase/reductase) family NAD(P)-dependent oxidoreductase similar to human biliverdin IX beta reductase (BVR-B, aka flavin reductase) that catalyzes the NADPH-dependent reduction of a variety of flavins, such as riboflavin, FAD or FMN, biliverdins, methemoglobin, and PQQ (pyrroloquinoline quinone); 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

Graphical summary

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List of domain hits

 Name Accession Description Interval E-value
BVR-B_like_SDR_a cd05244
biliverdin IX beta reductase (BVR-B, aka flavin reductase)-like proteins; atypical (a) SDRs; ...
 2-204 1.63e-64

biliverdin IX beta reductase (BVR-B, aka flavin reductase)-like proteins; atypical (a) SDRs; Human BVR-B catalyzes pyridine nucleotide-dependent production of bilirubin-IX beta during fetal development; in the adult BVR-B has flavin and ferric reductase activities. Human BVR-B catalyzes the reduction of FMN, FAD, and riboflavin. Recognition of flavin occurs mostly by hydrophobic interactions, accounting for the broad substrate specificity. Atypical SDRs are distinct from classical SDRs. BVR-B does not share the key catalytic triad, or conserved tyrosine typical of SDRs. The glycine-rich NADP-binding motif of BVR-B is GXXGXXG, which is similar but not identical to the pattern seen in extended SDRs. 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: 187555 [Multi-domain]  Cd Length: 207  Bit Score: 198.23  E-value: 1.63e-64
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    2 KIALLGASGRVGQAFLTQAAADeRFDIFALIRSQHADLPL-SKDRTVMGNARRLEDVKKIMENAEIVISCLGTDGDDT-- 78
Cdd:cd05244   1 KIAIIGATGRTGSAIVREALAR-GHEVTALVRDPAKLPAEhEKLKVVQGDVLDLEDVKEALEGQDAVISALGTRNDLSpt 79

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308   79 --LSTAMAHILSVMEEQHIKRLITIGTAGILDSRYEPGKYRFeTNESKRKQTRAAKEHAKVYEMLKESSLDWTIICPTYL 156
Cdd:cd05244  80 tlHSEGTRNIVSAMKAAGVKRLIVVGGAGSLDDRPKVTLVLD-TLLFPPALRRVAEDHARMLKVLRESGLDWTAVRPPAL 158

                       170       180       190       200
                ....*....|....*....|....*....|....*....|....*....
gi 2633308  157 PDGTATGVYRT-ERNVLPEGGTSISVGDTADFLYRELVTGEYVGNRVGL 204
Cdd:cd05244 159 FDGGATGGYYRvELLVDAKGGSRISRADLAIFMLDELETPEHVRKRPTI 207
 
Name Accession Description Interval E-value
BVR-B_like_SDR_a cd05244
biliverdin IX beta reductase (BVR-B, aka flavin reductase)-like proteins; atypical (a) SDRs; ...
 2-204 1.63e-64

biliverdin IX beta reductase (BVR-B, aka flavin reductase)-like proteins; atypical (a) SDRs; Human BVR-B catalyzes pyridine nucleotide-dependent production of bilirubin-IX beta during fetal development; in the adult BVR-B has flavin and ferric reductase activities. Human BVR-B catalyzes the reduction of FMN, FAD, and riboflavin. Recognition of flavin occurs mostly by hydrophobic interactions, accounting for the broad substrate specificity. Atypical SDRs are distinct from classical SDRs. BVR-B does not share the key catalytic triad, or conserved tyrosine typical of SDRs. The glycine-rich NADP-binding motif of BVR-B is GXXGXXG, which is similar but not identical to the pattern seen in extended SDRs. 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: 187555 [Multi-domain]  Cd Length: 207  Bit Score: 198.23  E-value: 1.63e-64
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    2 KIALLGASGRVGQAFLTQAAADeRFDIFALIRSQHADLPL-SKDRTVMGNARRLEDVKKIMENAEIVISCLGTDGDDT-- 78
Cdd:cd05244   1 KIAIIGATGRTGSAIVREALAR-GHEVTALVRDPAKLPAEhEKLKVVQGDVLDLEDVKEALEGQDAVISALGTRNDLSpt 79

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308   79 --LSTAMAHILSVMEEQHIKRLITIGTAGILDSRYEPGKYRFeTNESKRKQTRAAKEHAKVYEMLKESSLDWTIICPTYL 156
Cdd:cd05244  80 tlHSEGTRNIVSAMKAAGVKRLIVVGGAGSLDDRPKVTLVLD-TLLFPPALRRVAEDHARMLKVLRESGLDWTAVRPPAL 158

                       170       180       190       200
                ....*....|....*....|....*....|....*....|....*....
gi 2633308  157 PDGTATGVYRT-ERNVLPEGGTSISVGDTADFLYRELVTGEYVGNRVGL 204
Cdd:cd05244 159 FDGGATGGYYRvELLVDAKGGSRISRADLAIFMLDELETPEHVRKRPTI 207
YwnB COG2910
Putative NADH-flavin reductase [General function prediction only];
2-206 4.28e-61

Putative NADH-flavin reductase [General function prediction only];


Pssm-ID: 442154 [Multi-domain]  Cd Length: 205  Bit Score: 189.30  E-value: 4.28e-61
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    2 KIALLGASGRVGQAFLTQAAADErFDIFALIRS-QHADLPLSKDRTVMGNARRLEDVKKIMENAEIVISCLGTDGDDT-- 78
Cdd:COG2910   1 KIAVIGATGRVGSLIVREALARG-HEVTALVRNpEKLPDEHPGLTVVVGDVLDPAAVAEALAGADAVVSALGAGGGNPtt 79

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308   79 -LSTAMAHILSVMEEQHIKRLITIGTAGILDSRyePGKyRFETNESKRKQTRAAKEHAKVYEMLKESSLDWTIICPTYLP 157
Cdd:COG2910  80 vLSDGARALIDAMKAAGVKRLIVVGGAGSLDVA--PGL-GLDTPGFPAALKPAAAAKAAAEELLRASDLDWTIVRPAALT 156

                       170       180       190       200
                ....*....|....*....|....*....|....*....|....*....
gi 2633308  158 DGTATGVYRTERNVLPEGGTSISVGDTADFLYRELVTGEYVGNRVGLAY 206
Cdd:COG2910 157 DGERTGRYRLGGDGLLVDASSISRADVAVALLDELEDPAHIRQRFTVAY 205
NAD_binding_10 pfam13460
NAD(P)H-binding;
7-192 1.68e-36

NAD(P)H-binding;


Pssm-ID: 463885 [Multi-domain]  Cd Length: 183  Bit Score: 125.79  E-value: 1.68e-36
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308      7 GASGRVGQAfLTQAAADERFDIFALIRSQH--ADLP-LSKDRTVMGNARRLEDVKKIMENAEIVISCLGtdGDDTLSTAM 83
Cdd:pfam13460   1 GATGKIGRL-LVKQLLARGHEVTALVRNPEklADLEdHPGVEVVDGDVLDPDDLAEALAGQDAVISALG--GGGTDETGA 77

                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308     84 AHILSVMEEQHIKRLITIGTAGILDSRyePGKYRFETNESKRkqtRAAKEHAKVYEMLKESSLDWTIICPTYLPDGTATG 163
Cdd:pfam13460  78 KNIIDAAKAAGVKRFVLVSSLGVGDEV--PGPFGPWNKEMLG---PYLAAKRAAEELLRASGLDYTIVRPGWLTDGPTTG 152

                         170       180
                  ....*....|....*....|....*....
gi 2633308    164 VYRTERNvLPEGGTSISVGDTADFLYREL 192
Cdd:pfam13460 153 YRVTGKG-EPFKGGSISRADVADVLVALL 180
 
Name Accession Description Interval E-value
BVR-B_like_SDR_a cd05244
biliverdin IX beta reductase (BVR-B, aka flavin reductase)-like proteins; atypical (a) SDRs; ...
 2-204 1.63e-64

biliverdin IX beta reductase (BVR-B, aka flavin reductase)-like proteins; atypical (a) SDRs; Human BVR-B catalyzes pyridine nucleotide-dependent production of bilirubin-IX beta during fetal development; in the adult BVR-B has flavin and ferric reductase activities. Human BVR-B catalyzes the reduction of FMN, FAD, and riboflavin. Recognition of flavin occurs mostly by hydrophobic interactions, accounting for the broad substrate specificity. Atypical SDRs are distinct from classical SDRs. BVR-B does not share the key catalytic triad, or conserved tyrosine typical of SDRs. The glycine-rich NADP-binding motif of BVR-B is GXXGXXG, which is similar but not identical to the pattern seen in extended SDRs. 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: 187555 [Multi-domain]  Cd Length: 207  Bit Score: 198.23  E-value: 1.63e-64
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    2 KIALLGASGRVGQAFLTQAAADeRFDIFALIRSQHADLPL-SKDRTVMGNARRLEDVKKIMENAEIVISCLGTDGDDT-- 78
Cdd:cd05244   1 KIAIIGATGRTGSAIVREALAR-GHEVTALVRDPAKLPAEhEKLKVVQGDVLDLEDVKEALEGQDAVISALGTRNDLSpt 79

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308   79 --LSTAMAHILSVMEEQHIKRLITIGTAGILDSRYEPGKYRFeTNESKRKQTRAAKEHAKVYEMLKESSLDWTIICPTYL 156
Cdd:cd05244  80 tlHSEGTRNIVSAMKAAGVKRLIVVGGAGSLDDRPKVTLVLD-TLLFPPALRRVAEDHARMLKVLRESGLDWTAVRPPAL 158

                       170       180       190       200
                ....*....|....*....|....*....|....*....|....*....
gi 2633308  157 PDGTATGVYRT-ERNVLPEGGTSISVGDTADFLYRELVTGEYVGNRVGL 204
Cdd:cd05244 159 FDGGATGGYYRvELLVDAKGGSRISRADLAIFMLDELETPEHVRKRPTI 207
YwnB COG2910
Putative NADH-flavin reductase [General function prediction only];
2-206 4.28e-61

Putative NADH-flavin reductase [General function prediction only];


Pssm-ID: 442154 [Multi-domain]  Cd Length: 205  Bit Score: 189.30  E-value: 4.28e-61
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    2 KIALLGASGRVGQAFLTQAAADErFDIFALIRS-QHADLPLSKDRTVMGNARRLEDVKKIMENAEIVISCLGTDGDDT-- 78
Cdd:COG2910   1 KIAVIGATGRVGSLIVREALARG-HEVTALVRNpEKLPDEHPGLTVVVGDVLDPAAVAEALAGADAVVSALGAGGGNPtt 79

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308   79 -LSTAMAHILSVMEEQHIKRLITIGTAGILDSRyePGKyRFETNESKRKQTRAAKEHAKVYEMLKESSLDWTIICPTYLP 157
Cdd:COG2910  80 vLSDGARALIDAMKAAGVKRLIVVGGAGSLDVA--PGL-GLDTPGFPAALKPAAAAKAAAEELLRASDLDWTIVRPAALT 156

                       170       180       190       200
                ....*....|....*....|....*....|....*....|....*....
gi 2633308  158 DGTATGVYRTERNVLPEGGTSISVGDTADFLYRELVTGEYVGNRVGLAY 206
Cdd:COG2910 157 DGERTGRYRLGGDGLLVDASSISRADVAVALLDELEDPAHIRQRFTVAY 205
NAD_binding_10 pfam13460
NAD(P)H-binding;
7-192 1.68e-36

NAD(P)H-binding;


Pssm-ID: 463885 [Multi-domain]  Cd Length: 183  Bit Score: 125.79  E-value: 1.68e-36
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308      7 GASGRVGQAfLTQAAADERFDIFALIRSQH--ADLP-LSKDRTVMGNARRLEDVKKIMENAEIVISCLGtdGDDTLSTAM 83
Cdd:pfam13460   1 GATGKIGRL-LVKQLLARGHEVTALVRNPEklADLEdHPGVEVVDGDVLDPDDLAEALAGQDAVISALG--GGGTDETGA 77

                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308     84 AHILSVMEEQHIKRLITIGTAGILDSRyePGKYRFETNESKRkqtRAAKEHAKVYEMLKESSLDWTIICPTYLPDGTATG 163
Cdd:pfam13460  78 KNIIDAAKAAGVKRFVLVSSLGVGDEV--PGPFGPWNKEMLG---PYLAAKRAAEELLRASGLDYTIVRPGWLTDGPTTG 152

                         170       180
                  ....*....|....*....|....*....
gi 2633308    164 VYRTERNvLPEGGTSISVGDTADFLYREL 192
Cdd:pfam13460 153 YRVTGKG-EPFKGGSISRADVADVLVALL 180
SDR_a6 cd05267
atypical (a) SDRs, subgroup 6; These atypical SDR family members of unknown function have only ...
 1-205 7.66e-19

atypical (a) SDRs, subgroup 6; These atypical SDR family members of unknown function have only a partial match to a prototypical glycine-rich NAD(P)-binding motif consensus, GXXG, which conserves part of the motif of extended SDR. Furthermore, they lack the characteristic active site residues of the SDRs. This subgroup is related to phenylcoumaran benzylic ether reductase, an NADPH-dependent aromatic alcohol reductase. One member is identified as a putative NAD-dependent epimerase/dehydratase. 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: 187577 [Multi-domain]  Cd Length: 203  Bit Score: 80.48  E-value: 7.66e-19
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    1 MKIALLGASGRVGQAFLTQAAADERFDIFALIRSQHADLPLSKDRT--VMGNARRLEDVKKIMENAEIVISCLGtdgDDT 78
Cdd:cd05267   1 KKVLILGANGEIAREATTMLLENSNVELTLFLRNAHRLLHLKSARVtvVEGDALNSDDLKAAMRGQDVVYANLG---GTD 77

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308   79 LSTAMAHILSVMEEQHIKRLITIGTAGILDSRYEP-GKYRFETNESKRKQTRAAkehAKVYEmlkESSLDWTIICPTYLP 157
Cdd:cd05267  78 LDQQAENVVQAMKAVGVKRLIWTTSLGIYDEVPGKfGEWNKEFIGNYLAPYRKS---AAVIE---NSDLDYTLLRPAWLT 151

                       170       180       190       200       210
                ....*....|....*....|....*....|....*....|....*....|
gi 2633308  158 DGTaTGVYRTERNVLPEGGTSISVGDTADFLYrELVTGE--YVGNRVGLA 205
Cdd:cd05267 152 NND-EIDYELTPKGEAFKGTEVSRKSVADLIT-DIINHPdyHVRESIGIN 199
YbjT COG0702
Uncharacterized conserved protein YbjT, contains NAD(P)-binding and DUF2867 domains [General ...
 2-205 3.80e-16

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: 73.34  E-value: 3.80e-16
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    2 KIALLGASGRVGQAfLTQAAADERFDIFALIRS--QHADLPLSKDRTVMGNARRLEDVKKIMENAEIVISCLGTDGDDTL 79
Cdd:COG0702   1 KILVTGATGFIGRR-VVRALLARGHPVRALVRDpeKAAALAAAGVEVVQGDLDDPESLAAALAGVDAVFLLVPSGPGGDF 79

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308   80 S---TAMAHILSVMEEQHIKRLITIGTAGIldsryepgkyrfetneSKRKQTRAAKEHAKVYEMLKESSLDWTIICPT-- 154
Cdd:COG0702  80 AvdvEGARNLADAAKAAGVKRIVYLSALGA----------------DRDSPSPYLRAKAAVEEALRASGLPYTILRPGwf 143

                       170       180       190       200       210       220
                ....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308  155 ------YLPDGTATGVYRternvLPEGGT---SISVGDTADFLYRELVTGEYVGNRVGLA 205
Cdd:COG0702 144 mgnllgFFERLRERGVLP-----LPAGDGrvqPIAVRDVAEAAAAALTDPGHAGRTYELG 198
SDR_a5 cd05243
atypical (a) SDRs, subgroup 5; This subgroup contains atypical SDRs, some of which are ...
 2-188 5.57e-14

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: 67.65  E-value: 5.57e-14
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    2 KIALLGASGRVGQaFLTQAAADERFDIFALIR--SQHADLPLSKDRTVMGNARRLEDVKKIMENAEIVISCLGTDGDDTL 79
Cdd:cd05243   1 KVLVVGATGKVGR-HVVRELLDRGYQVRALVRdpSQAEKLEAAGAEVVVGDLTDAESLAAALEGIDAVISAAGSGGKGGP 79

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308   80 ST------AMAHILSVMEEQHIKRLITIGTAGILDSRYEPG--------KYRFEtneskrkqtraakehakvyEMLKESS 145
Cdd:cd05243  80 RTeavdydGNINLIDAAKKAGVKRFVLVSSIGADKPSHPLEalgpyldaKRKAE-------------------DYLRASG 140

                       170       180       190       200
                ....*....|....*....|....*....|....*....|....*
gi 2633308  146 LDWTIICPTYLPDGT-ATG-VYRTERNVLPEGgtSISVGDTADFL 188
Cdd:cd05243 141 LDYTIVRPGGLTDDPaGTGrVVLGGDGTRLDG--PISRADVAEVL 183
SDR_e_a cd05226
Extended (e) and atypical (a) SDRs; Extended or atypical short-chain dehydrogenases/reductases ...
 3-199 1.78e-10

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: 57.41  E-value: 1.78e-10
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    3 IALLGASGRVGQAfLTQAAADERFDIFALIRSQHADLPLSKDRT--VMGNARRLEDVKKIMENAEIVISCLGTDGDD--- 77
Cdd:cd05226   1 ILILGATGFIGRA-LARELLEQGHEVTLLVRNTKRLSKEDQEPVavVEGDLRDLDSLSDAVQGVDVVIHLAGAPRDTrdf 79

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308   78 --TLSTAMAHILSVMEEQHIKRLITIGTAGILDSRYEpgkyrfETNESKRKQTRAAKehAKVYEMLKESSLDWTIICPty 155
Cdd:cd05226  80 ceVDVEGTRNVLEAAKEAGVKHFIFISSLGAYGDLHE------ETEPSPSSPYLAVK--AKTEAVLREASLPYTIVRP-- 149

                       170       180       190       200
                ....*....|....*....|....*....|....*....|....
gi 2633308  156 lpdgtatgvyrternvlpeggtSISVGDTADFLYRELVTGEYVG 199
Cdd:cd05226 150 ----------------------GVIYGDLARAIANAVVTPGKKN 171
PCBER_SDR_a cd05259
phenylcoumaran benzylic ether reductase (PCBER) like, atypical (a) SDRs; PCBER and ...
 2-202 4.60e-07

phenylcoumaran benzylic ether reductase (PCBER) like, atypical (a) SDRs; PCBER and pinoresinol-lariciresinol reductases are NADPH-dependent aromatic alcohol reductases, and are atypical members of the SDR family. Other proteins in this subgroup are identified as eugenol synthase. These proteins contain an N-terminus characteristic of NAD(P)-binding proteins and a small C-terminal domain presumed to be involved in substrate binding, but they do not have the conserved active site Tyr residue typically found in SDRs. Numerous other members have unknown functions. The glycine rich NADP-binding motif in this subgroup is of 2 forms: GXGXXG and G[GA]XGXXG; it tends to be atypical compared with the forms generally seen in classical or extended SDRs. The usual SDR active site tetrad is not present, but a critical active site Lys at the usual SDR position has been identified in various members, though other charged and polar residues are found at this position in this subgroup. Atypical SDR-related proteins retain the Rossmann fold of the SDRs, but have limited sequence identity and generally lack the catalytic properties of the archetypical members. 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: 187569 [Multi-domain]  Cd Length: 282  Bit Score: 48.84  E-value: 4.60e-07
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    2 KIALLGASGRVGQAFLTQAAADERFDIFALIRS---QHADLPLSKDRTVMGNARRLEDVKKIMENAEIVISCLGTDGDDT 78
Cdd:cd05259   1 KIAIAGATGTLGGPIVSALLASPGFTVTVLTRPsstSSNEFQPSGVKVVPVDYASHESLVAALKGVDAVISALGGAAIGD 80

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308   79 lstamahilsvmeeqHIKRLITIGTAGIldSRYEPGKYRF-ETNESKRKQTRAAKEHAKVYEMLKESS--LDWTIICP-- 153
Cdd:cd05259  81 ---------------QLKLIDAAIAAGV--KRFIPSEFGVdYDRIGALPLLDLFDEKRDVRRYLRAKNagLPWTYVSTgm 143

                       170       180       190       200       210
                ....*....|....*....|....*....|....*....|....*....|....*.
gi 2633308  154 ---TYLPDGTATGVYRTERNVLPEGG----TSISVGDTADFLYRELVTGEYVGNRV 202
Cdd:cd05259 144 fldYLLEPLFGVVDLANRTATIYGDGetkfAFTTLEDIGRAVARALTHPDRTLNRV 199
NmrA pfam05368
NmrA-like family; NmrA is a negative transcriptional regulator involved in the ...
 3-154 6.02e-05

NmrA-like family; NmrA is a negative transcriptional regulator involved in the post-translational modification of the transcription factor AreA. NmrA is part of a system controlling nitrogen metabolite repression in fungi. This family only contains a few sequences as iteration results in significant matches to other Rossmann fold families.


Pssm-ID: 398829 [Multi-domain]  Cd Length: 236  Bit Score: 42.33  E-value: 6.02e-05
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308      3 IALLGASGRVGqAFLTQAAADERFDIFALIRSQHADLPLS-KDR---TVMGNARRLEDVKKIMENAEIVISCLGTDGDDT 78
Cdd:pfam05368   1 ILVFGATGQQG-GSVVRASLKAGHKVRALVRDPKSELAKSlKEAgveLVKGDLDDKESLVEALKGVDVVFSVTGFWAGKE 79

                          90       100       110       120       130       140       150
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*...
gi 2633308     79 LSTAMAhILSVMEEQHIKRLI--TIGTAGILDSRYEPGKYRFetnESKrkqtraakehAKVYEMLKESSLDWTIICPT 154
Cdd:pfam05368  80 IEDGKK-LADAAKEAGVKHFIpsSFGNDNDISNGVEPAVPHF---DSK----------AEIERYIRALGIPYTFVYAG 143
SDR_a3 cd05229
atypical (a) SDRs, subgroup 3; These atypical SDR family members of unknown function have a ...
 2-74 3.52e-04

atypical (a) SDRs, subgroup 3; These atypical SDR family members of unknown function have a glycine-rich NAD(P)-binding motif consensus that is very similar to the extended SDRs, GXXGXXG. Generally, this group has poor conservation of the active site tetrad, However, individual sequences do contain matches to the YXXXK active site motif, and generally Tyr or Asn in place of the upstream Ser found in most SDRs. 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: 187540 [Multi-domain]  Cd Length: 302  Bit Score: 40.39  E-value: 3.52e-04
                        10        20        30        40        50        60        70
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|...
gi 2633308    2 KIALLGASGRVGQAfLTQAAADERFDIFALIRSQHADLPLSKDRTVMGNARRLEDVKKIMENAEIVISCLGTD 74
Cdd:cd05229   1 TAHVLGASGPIGRE-VARELRRRGWDVRLVSRSGSKLAWLPGVEIVAADAMDASSVIAAARGADVIYHCANPA 72
DapB COG0289
4-hydroxy-tetrahydrodipicolinate reductase [Amino acid transport and metabolism]; ...
 1-112 5.25e-04

4-hydroxy-tetrahydrodipicolinate reductase [Amino acid transport and metabolism]; 4-hydroxy-tetrahydrodipicolinate reductase is part of the Pathway/BioSystem: Lysine biosynthesis


Pssm-ID: 440058 [Multi-domain]  Cd Length: 257  Bit Score: 39.72  E-value: 5.25e-04
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    1 MKIALLGASGRVGQAFLTQAAADERFDI-FALIRSQHADLPLSkdrTVMGNARRLEDVKKIMENAEIVIsclgtdgDDTL 79
Cdd:COG0289   1 IKIAVAGASGRMGRELIRAVLEAPDLELvAAIDRPGSPGQDAG---ELALGVPVTDDLEEALAKADVVI-------DFTH 70

                        90       100       110
                ....*....|....*....|....*....|....
gi 2633308   80 -STAMAHILSVMEeqHIKRLItIGTAGILDSRYE 112
Cdd:COG0289  71 pEATLENLEAALE--AGVPVV-IGTTGFSEEQLA 101
Semialdhyde_dh pfam01118
Semialdehyde dehydrogenase, NAD binding domain; This Pfam entry contains the following members: ...
 2-72 7.66e-04

Semialdehyde dehydrogenase, NAD binding domain; This Pfam entry contains the following members: N-acetyl-glutamine semialdehyde dehydrogenase (AgrC) Aspartate-semialdehyde dehydrogenase


Pssm-ID: 426059 [Multi-domain]  Cd Length: 121  Bit Score: 37.89  E-value: 7.66e-04
                          10        20        30        40        50        60        70
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*
gi 2633308      2 KIALLGASGRVGQAFLTQAAADERFDIFALI-RSQHADLPLSKDRTVMGNAR--RLEDVK-KIMENAEIVISCLG 72
Cdd:pfam01118   1 KVAIVGATGYVGQELLRLLEEHPPVELVVLFaSSRSAGKKLAFVHPILEGGKdlVVEDVDpEDFKDVDIVFFALP 75
NDUFA9_like_SDR_a cd05271
NADH dehydrogenase (ubiquinone) 1 alpha subcomplex, subunit 9, 39 kDa, (NDUFA9) -like, ...
 1-196 2.36e-03

NADH dehydrogenase (ubiquinone) 1 alpha subcomplex, subunit 9, 39 kDa, (NDUFA9) -like, atypical (a) SDRs; This subgroup of extended SDR-like proteins are atypical SDRs. They have a glycine-rich NAD(P)-binding motif similar to the typical SDRs, GXXGXXG, and have the YXXXK active site motif (though not the other residues of the SDR tetrad). Members identified include NDUFA9 (mitochondrial) and putative nucleoside-diphosphate-sugar epimerase. 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: 187579 [Multi-domain]  Cd Length: 273  Bit Score: 38.00  E-value: 2.36e-03
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    1 MKIALLGASGRVGQaFLTQAAADERFDIFALIRS--QHADLPLSKD----RTVMGNARRLEDVKKIMENAEIVISCLGTD 74
Cdd:cd05271   1 MVVTVFGATGFIGR-YVVNRLAKRGSQVIVPYRCeaYARRLLVMGDlgqvLFVEFDLRDDESIRKALEGSDVVINLVGRL 79

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308   75 ---GDDTLSTAMAHILS----VMEEQHIKRLITIGTAGI-LDSryepgkyrfetnESKRKQTRAAKEHAkvyemLKESSL 146
Cdd:cd05271  80 yetKNFSFEDVHVEGPErlakAAKEAGVERLIHISALGAdANS------------PSKYLRSKAEGEEA-----VREAFP 142

                       170       180       190       200       210       220
                ....*....|....*....|....*....|....*....|....*....|....*....|.
gi 2633308  147 DWTIICPTYL--PDG-----TATGVYRTERNVLPEGGTS----ISVGDTADFLYRELVTGE 196
Cdd:cd05271 143 EATIVRPSVVfgREDrflnrFAKLLAFLPFPPLIGGGQTkfqpVYVGDVAEAIARALKDPE 203
ASADH_N_like cd24147
N-terminal NAD(P)-binding domain of aspartate beta-semialdehyde dehydrogenase (ASADH), USG-1 ...
 1-74 2.96e-03

N-terminal NAD(P)-binding domain of aspartate beta-semialdehyde dehydrogenase (ASADH), USG-1 protein and similar proteins; The family includes aspartate beta-semialdehyde dehydrogenase (ASADH), NADP-dependent malonyl-CoA reductase (MCR), and USG-1 protein. They contain an N-terminal Rossmann fold NAD(P) binding domain and a C-terminal glyceraldehyde-3-phosphate dehydrogenase (GAPDH)-like domain and are members of the GAPDH superfamily of proteins. ASADH (EC 1.2.1.11), also called ASA dehydrogenase (ASD), or aspartate-beta-semialdehyde dehydrogenase, catalyzes the NADPH-dependent formation of L-aspartate-semialdehyde (ASA) by the reductive dephosphorylation of L-aspartyl-4-phosphate, which is the second step of the aspartate biosynthetic pathway. ASA can either be further reduced to homoserine, which leads to methionine, threonine, or isoleucine, or it can be condensed with pyruvate and cyclized into dihydrodipicolinate, and then converted into diaminopimelate, a component of bacterial cell walls, and finally decarboxylated to produce lysine. NADP-dependent MCR (EC 1.2.1.75) is mainly found in Archaea. It catalyzes the reduction of malonyl-CoA to malonate semialdehyde, a key step in the 3-hydroxypropanoate and the 3-hydroxypropanoate/4-hydroxybutyrate cycles. It can also use succinyl-CoA and succinate semialdehyde as substrates but at a lower rate than malonyl-CoA. Sequence comparison suggests that the archaeal MCR gene (mcr) has evolved from the duplication of a common ancestral ASADH gene (asd). The biological function of USG-1 protein and homologs remains unclear. They are homologs to ASADH but lack the conserved active site residues of the ASADH protein C-terminal catalytic domain.


Pssm-ID: 467523 [Multi-domain]  Cd Length: 142  Bit Score: 36.55  E-value: 2.96e-03
                        10        20        30        40        50        60        70
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*...
gi 2633308    1 MKIALLGASGRVGQAFLtQAAADERFDIF---ALIRSQHADLPlSKDRtvmGNARRLEDVKKI-MENAEIVISCLGTD 74
Cdd:cd24147   1 LRVGVVGATGAVGSEIL-QLLAEEPDPLFelrALASEESAGKK-AEFA---GEAIMVQEADPIdFLGLDIVFLCAGAG 73
SDR_a2 cd05245
atypical (a) SDRs, subgroup 2; This subgroup contains atypical SDRs, one member is identified ...
 3-115 8.23e-03

atypical (a) SDRs, subgroup 2; This subgroup contains atypical SDRs, one member is identified as Escherichia coli protein ybjT, function unknown. Atypical SDRs are distinct from classical SDRs. Members of this subgroup have a glycine-rich NAD(P)-binding motif consensus that generally matches the extended SDRs, TGXXGXXG, but lacks the characteristic active site residues of the SDRs. This subgroup has basic residues (HXXXR) in place of the active site motif YXXXK, these may have a catalytic role. 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: 187556 [Multi-domain]  Cd Length: 293  Bit Score: 36.17  E-value: 8.23e-03
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 2633308    3 IALLGASGRVGQAfLTQAAADERFDIFALIRSQH--ADLPLSKDRTVM-GNARRLEDVKKIMENAEIV---ISCLGTDGD 76
Cdd:cd05245   1 VLVTGATGYVGGR-LVPRLLQEGHQVRALVRSPEklADRPWSERVTVVrGDLEDPESLRAALEGIDTAyylVHSMGSGGD 79

                        90       100       110       120       130
                ....*....|....*....|....*....|....*....|....*....|.
gi 2633308   77 --DTLSTAMAHILSVMEEQHIKRLITIGtaGI----------LDSRYEPGK 115
Cdd:cd05245  80 feEADRRAARNFARAARAAGVKRIIYLG--GLipkgeelsphLRSRAEVGE 128
 
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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