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Conserved domains on  [gi|50284885|ref|XP_444870|]
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YPS7 [Nakaseomyces glabratus]

Protein Classification

pepsin/retropepsin-like aspartic protease family protein( domain architecture ID 27721)

pepsin/retropepsin-like aspartic protease family protein

Graphical summary

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List of domain hits

 Name Accession Description Interval E-value
pepsin_retropepsin_like super family cl11403
Cellular and retroviral pepsin-like aspartate proteases; This family includes both cellular ...
 149-426 4.93e-28

Cellular and retroviral pepsin-like aspartate proteases; This family includes both cellular and retroviral pepsin-like aspartate proteases. The cellular pepsin and pepsin-like enzymes are twice as long as their retroviral counterparts. The cellular pepsin-like aspartic proteases are found in mammals, plants, fungi and bacteria. These well known and extensively characterized enzymes include pepsins, chymosin, rennin, cathepsins, and fungal aspartic proteases. Several have long been known to be medically (rennin, cathepsin D and E, pepsin) or commercially (chymosin) important. The eukaryotic pepsin-like proteases contain two domains possessing similar topological features. The N- and C-terminal domains, although structurally related by a 2-fold axis, have only limited sequence homology except in the vicinity of the active site. This suggests that the enzymes evolved by an ancient duplication event. The eukaryotic pepsin-like proteases have two active site ASP residues with each N- and C-terminal lobe contributing one residue. While the fungal and mammalian pepsins are bilobal proteins, retropepsins function as dimers and the monomer resembles structure of the N- or C-terminal domains of eukaryotic enzyme. The active site motif (Asp-Thr/Ser-Gly-Ser) is conserved between the retroviral and eukaryotic proteases and between the N-and C-terminal of eukaryotic pepsin-like proteases. The retropepsin-like family includes pepsin-like aspartate proteases from retroviruses, retrotransposons and retroelements; as well as eukaryotic DNA-damage-inducible proteins (DDIs), and bacterial aspartate peptidases. Retropepsin is synthesized as part of the POL polyprotein that contains an aspartyl-protease, a reverse transcriptase, RNase H, and an integrase. The POL polyprotein undergoes specific enzymatic cleavage to yield the mature proteins. This family of aspartate proteases is classified by MEROPS as the peptidase family A1 (pepsin A) and A2 (retropepsin family).


The actual alignment was detected with superfamily member cd05474:

Pssm-ID: 472175 [Multi-domain]  Cd Length: 295  Bit Score: 114.20  E-value: 4.93e-28
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 149 VSFRNHTLTvqNLSFFNADYSSGyLYGSLGLGgtlnsDTELEGDFINHSFF--FLDALKEARLINSSSYSLWLGSQKrng 226
Cdd:cd05474  51 VSIGGATVK--NLQFAVANSTSS-DVGVLGIG-----LPGNEATYGTGYTYpnFPIALKKQGLIKKNAYSLYLNDLD--- 119

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 227 fADTsdaneaGYLIFGAVDPNLVEGEFRKFDMIPyihpQTGKVAYGYPVVPMGPIYITSSSGrslNVTTDGFSAPVLLDP 306
Cdd:cd05474 120 -AST------GSILFGGVDTAKYSGDLVTLPIVN----DNGGSEPSELSVTLSSISVNGSSG---NTTLLSKNLPALLDS 185

                       170       180       190       200       210       220       230       240
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 307 SFALSYLPTKAIIQIAIQIAAVYVESLDLWLVSCDVASSGaTVDFSFGDLTIKVPLSDLLASTHDQstnttlhfNTGQEA 386
Cdd:cd05474 186 GTTLTYLPSDIVDAIAKQLGATYDSDEGLYVVDCDAKDDG-SLTFNFGGATISVPLSDLVLPASTD--------DGGDGA 256

                       250       260       270       280
                ....*....|....*....|....*....|....*....|
gi 50284885 387 CVLQLYPNTfTGYNVLGQAFMKNAYLAVDLEGKGVAMGQA 426
Cdd:cd05474 257 CYLGIQPST-SDYNILGDTFLRSAYVVYDLDNNEISLAQA 295
 
Name Accession Description Interval E-value
SAP_like cd05474
SAPs, pepsin-like proteinases secreted from pathogens to degrade host proteins; SAPs (Secreted ...
 149-426 4.93e-28

SAPs, pepsin-like proteinases secreted from pathogens to degrade host proteins; SAPs (Secreted aspartic proteinases) are secreted from a group of pathogenic fungi, predominantly Candida species. They are secreted from the pathogen to degrade host proteins. SAP is one of the most significant extracellular hydrolytic enzymes produced by C. albicans. SAP proteins, encoded by a family of 10 SAP genes. All 10 SAP genes of C. albicans encode preproenzymes, approximately 60 amino acid longer than the mature enzyme, which are processed when transported via the secretory pathway. The mature enzymes contain sequence motifs typical for all aspartyl proteinases, including the two conserved aspartate residues other active site and conserved cysteine residues implicated in the maintenance of the three-dimensional structure. Most Sap proteins contain putative N-glycosylation sites, but it remains to be determined which Sap proteins are glycosylated. This family of aspartate proteases is classified by MEROPS as the peptidase family A1 (pepsin A, clan AA). The overall structure of Sap protein conforms to the classical aspartic proteinase fold typified by pepsin. SAP is a bilobal enzyme, each lobe contributing a catalytic Asp residue, with an extended active site cleft localized between the two lobes of the molecule. One lobe may be evolved from the other through ancient gene-duplication event. More recently evolved enzymes have similar three-dimensional structures, however their amino acid sequences are more divergent except for the conserved catalytic site motif. This family of aspartate proteases is classified by MEROPS as the peptidase family A1 (pepsin A, clan AA).


Pssm-ID: 133141 [Multi-domain]  Cd Length: 295  Bit Score: 114.20  E-value: 4.93e-28
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 149 VSFRNHTLTvqNLSFFNADYSSGyLYGSLGLGgtlnsDTELEGDFINHSFF--FLDALKEARLINSSSYSLWLGSQKrng 226
Cdd:cd05474  51 VSIGGATVK--NLQFAVANSTSS-DVGVLGIG-----LPGNEATYGTGYTYpnFPIALKKQGLIKKNAYSLYLNDLD--- 119

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 227 fADTsdaneaGYLIFGAVDPNLVEGEFRKFDMIPyihpQTGKVAYGYPVVPMGPIYITSSSGrslNVTTDGFSAPVLLDP 306
Cdd:cd05474 120 -AST------GSILFGGVDTAKYSGDLVTLPIVN----DNGGSEPSELSVTLSSISVNGSSG---NTTLLSKNLPALLDS 185

                       170       180       190       200       210       220       230       240
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 307 SFALSYLPTKAIIQIAIQIAAVYVESLDLWLVSCDVASSGaTVDFSFGDLTIKVPLSDLLASTHDQstnttlhfNTGQEA 386
Cdd:cd05474 186 GTTLTYLPSDIVDAIAKQLGATYDSDEGLYVVDCDAKDDG-SLTFNFGGATISVPLSDLVLPASTD--------DGGDGA 256

                       250       260       270       280
                ....*....|....*....|....*....|....*....|
gi 50284885 387 CVLQLYPNTfTGYNVLGQAFMKNAYLAVDLEGKGVAMGQA 426
Cdd:cd05474 257 CYLGIQPST-SDYNILGDTFLRSAYVVYDLDNNEISLAQA 295
Asp pfam00026
Eukaryotic aspartyl protease; Aspartyl (acid) proteases include pepsins, cathepsins, and ...
 49-426 2.07e-19

Eukaryotic aspartyl protease; Aspartyl (acid) proteases include pepsins, cathepsins, and renins. Two-domain structure, probably arising from ancestral duplication. This family does not include the retroviral nor retrotransposon proteases (pfam00077), which are much smaller and appear to be homologous to a single domain of the eukaryotic asp proteases.


Pssm-ID: 394983 [Multi-domain]  Cd Length: 313  Bit Score: 89.26  E-value: 2.07e-19
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885    49 YYVNATLGTPGQWQQLGLGLAQPYVWVVSgdadSQCNRlDSGCLSGPLYYPQESRTSSTGGDKYSINFIDGiSLNGTRYM 128
Cdd:pfam00026   2 YFGTISIGTPPQKFTVIFDTGSSDLWVPS----SYCTK-SSACKSHGTFDPSSSSTYKLNGTTFSISYGDG-SASGFLGQ 75

                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885   129 DvmrlmnvssSLNVSGvdsgvsfrnhtLTVQNLSFFNADYSSGYLY------GSLGLGGTLNSDTELEgdfinhsfFFLD 202
Cdd:pfam00026  76 D---------TVTVGG-----------LTITNQEFGLATKEPGSFFeyakfdGILGLGFPSISAVGAT--------PVFD 127

                         170       180       190       200       210       220       230       240
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885   203 ALKEARLINSSSYSLWLGSqkrngfadtsDANEAGYLIFGAVDPNLVEGEFRKFDMipyihpqtgkVAYGYPVVPMGPIY 282
Cdd:pfam00026 128 NLKSQGLIDSPAFSVYLNS----------PDAAGGEIIFGGVDPSKYTGSLTYVPV----------TSQGYWQITLDSVT 187

                         250       260       270       280       290       300       310       320
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885   283 ITSSSgrslNVTTDGFSApvLLDPSFALSYLPTKAIIQIAIQIAAVYVESlDLWLVSCDVASSGATVDFSFGDLTIKVPL 362
Cdd:pfam00026 188 VGGST----SACSSGCQA--ILDTGTSLLYGPTSIVSKIAKAVGASSSEY-GEYVVDCDSISTLPDITFVIGGAKITVPP 260

                         330       340       350       360       370       380
                  ....*....|....*....|....*....|....*....|....*....|....*....|....
gi 50284885   363 SDLlasthdqstntTLHFNTGQEACVLQLYPNTFTGYNVLGQAFMKNAYLAVDLEGKGVAMGQA 426
Cdd:pfam00026 261 SAY-----------VLQNSQGGSTCLSGFQPPPGGPLWILGDVFLRSAYVVFDRDNNRIGFAPA 313
 
Name Accession Description Interval E-value
SAP_like cd05474
SAPs, pepsin-like proteinases secreted from pathogens to degrade host proteins; SAPs (Secreted ...
 149-426 4.93e-28

SAPs, pepsin-like proteinases secreted from pathogens to degrade host proteins; SAPs (Secreted aspartic proteinases) are secreted from a group of pathogenic fungi, predominantly Candida species. They are secreted from the pathogen to degrade host proteins. SAP is one of the most significant extracellular hydrolytic enzymes produced by C. albicans. SAP proteins, encoded by a family of 10 SAP genes. All 10 SAP genes of C. albicans encode preproenzymes, approximately 60 amino acid longer than the mature enzyme, which are processed when transported via the secretory pathway. The mature enzymes contain sequence motifs typical for all aspartyl proteinases, including the two conserved aspartate residues other active site and conserved cysteine residues implicated in the maintenance of the three-dimensional structure. Most Sap proteins contain putative N-glycosylation sites, but it remains to be determined which Sap proteins are glycosylated. This family of aspartate proteases is classified by MEROPS as the peptidase family A1 (pepsin A, clan AA). The overall structure of Sap protein conforms to the classical aspartic proteinase fold typified by pepsin. SAP is a bilobal enzyme, each lobe contributing a catalytic Asp residue, with an extended active site cleft localized between the two lobes of the molecule. One lobe may be evolved from the other through ancient gene-duplication event. More recently evolved enzymes have similar three-dimensional structures, however their amino acid sequences are more divergent except for the conserved catalytic site motif. This family of aspartate proteases is classified by MEROPS as the peptidase family A1 (pepsin A, clan AA).


Pssm-ID: 133141 [Multi-domain]  Cd Length: 295  Bit Score: 114.20  E-value: 4.93e-28
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 149 VSFRNHTLTvqNLSFFNADYSSGyLYGSLGLGgtlnsDTELEGDFINHSFF--FLDALKEARLINSSSYSLWLGSQKrng 226
Cdd:cd05474  51 VSIGGATVK--NLQFAVANSTSS-DVGVLGIG-----LPGNEATYGTGYTYpnFPIALKKQGLIKKNAYSLYLNDLD--- 119

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 227 fADTsdaneaGYLIFGAVDPNLVEGEFRKFDMIPyihpQTGKVAYGYPVVPMGPIYITSSSGrslNVTTDGFSAPVLLDP 306
Cdd:cd05474 120 -AST------GSILFGGVDTAKYSGDLVTLPIVN----DNGGSEPSELSVTLSSISVNGSSG---NTTLLSKNLPALLDS 185

                       170       180       190       200       210       220       230       240
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 307 SFALSYLPTKAIIQIAIQIAAVYVESLDLWLVSCDVASSGaTVDFSFGDLTIKVPLSDLLASTHDQstnttlhfNTGQEA 386
Cdd:cd05474 186 GTTLTYLPSDIVDAIAKQLGATYDSDEGLYVVDCDAKDDG-SLTFNFGGATISVPLSDLVLPASTD--------DGGDGA 256

                       250       260       270       280
                ....*....|....*....|....*....|....*....|
gi 50284885 387 CVLQLYPNTfTGYNVLGQAFMKNAYLAVDLEGKGVAMGQA 426
Cdd:cd05474 257 CYLGIQPST-SDYNILGDTFLRSAYVVYDLDNNEISLAQA 295
pepsin_like cd05471
Pepsin-like aspartic proteases, bilobal enzymes that cleave bonds in peptides at acidic pH; ...
 49-419 5.33e-23

Pepsin-like aspartic proteases, bilobal enzymes that cleave bonds in peptides at acidic pH; Pepsin-like aspartic proteases are found in mammals, plants, fungi and bacteria. These well known and extensively characterized enzymes include pepsins, chymosin, renin, cathepsins, and fungal aspartic proteases. Several have long been known to be medically (renin, cathepsin D and E, pepsin) or commercially (chymosin) important. Structurally, aspartic proteases are bilobal enzymes, each lobe contributing a catalytic Aspartate residue, with an extended active site cleft localized between the two lobes of the molecule. The N- and C-terminal domains, although structurally related by a 2-fold axis, have only limited sequence homology except the vicinity of the active site. This suggests that the enzymes evolved by an ancient duplication event. Most members of the pepsin family specifically cleave bonds in peptides that are at least six residues in length, with hydrophobic residues in both the P1 and P1' positions. The active site is located at the groove formed by the two lobes, with an extended loop projecting over the cleft to form an 11-residue flap, which encloses substrates and inhibitors in the active site. Specificity is determined by nearest-neighbor hydrophobic residues surrounding the catalytic aspartates, and by three residues in the flap.The enzymes are mostly secreted from cells as inactive proenzymes that activate autocatalytically at acidic pH. This family of aspartate proteases is classified by MEROPS as the peptidase family A1 (pepsin A, clan AA).


Pssm-ID: 133138 [Multi-domain]  Cd Length: 283  Bit Score: 99.04  E-value: 5.33e-23
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885  49 YYVNATLGTPGQWQQLGLGLAQPYVWVVSgdadSQCNRLDSGCLSGPLYYPQESRTSSTGGDKYSINFIDGiSLNGTRYM 128
Cdd:cd05471   1 YYGEITIGTPPQKFSVIFDTGSSLLWVPS----SNCTSCSCQKHPRFKYDSSKSSTYKDTGCTFSITYGDG-SVTGGLGT 75

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 129 DVMRLMNvssslnvsgvdsgvsfrnhtLTVQNLSFFNADYSSGYLY-----GSLGLGGTLNSdtelegdfINHSFFFLDA 203
Cdd:cd05471  76 DTVTIGG--------------------LTIPNQTFGCATSESGDFSssgfdGILGLGFPSLS--------VDGVPSFFDQ 127

                       170       180       190       200       210       220       230       240
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 204 LKEARLINSSSYSLWLGSQkrngfadtSDANEAGYLIFGAVDPNLVEGEFRKFDMIPYihpqtgkvAYGYPVVPMGPIYI 283
Cdd:cd05471 128 LKSQGLISSPVFSFYLGRD--------GDGGNGGELTFGGIDPSKYTGDLTYTPVVSN--------GPGYWQVPLDGISV 191

                       250       260       270       280       290       300       310       320
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 284 TSSSgrslnVTTDGFSAPVLLDPSFALSYLPTKAIIQIAIQIAAVYVESLDLWLVSCDVASSGATVDFSFgdltikvpls 363
Cdd:cd05471 192 GGKS-----VISSSGGGGAIVDSGTSLIYLPSSVYDAILKALGAAVSSSDGGYGVDCSPCDTLPDITFTF---------- 256

                       330       340       350       360       370
                ....*....|....*....|....*....|....*....|....*....|....*.
gi 50284885 364 dllasthdqstnttlhfntgqeacvlqlypntftgYNVLGQAFMKNAYLAVDLEGK 419
Cdd:cd05471 257 -----------------------------------LWILGDVFLRNYYTVFDLDNN 277
Asp pfam00026
Eukaryotic aspartyl protease; Aspartyl (acid) proteases include pepsins, cathepsins, and ...
 49-426 2.07e-19

Eukaryotic aspartyl protease; Aspartyl (acid) proteases include pepsins, cathepsins, and renins. Two-domain structure, probably arising from ancestral duplication. This family does not include the retroviral nor retrotransposon proteases (pfam00077), which are much smaller and appear to be homologous to a single domain of the eukaryotic asp proteases.


Pssm-ID: 394983 [Multi-domain]  Cd Length: 313  Bit Score: 89.26  E-value: 2.07e-19
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885    49 YYVNATLGTPGQWQQLGLGLAQPYVWVVSgdadSQCNRlDSGCLSGPLYYPQESRTSSTGGDKYSINFIDGiSLNGTRYM 128
Cdd:pfam00026   2 YFGTISIGTPPQKFTVIFDTGSSDLWVPS----SYCTK-SSACKSHGTFDPSSSSTYKLNGTTFSISYGDG-SASGFLGQ 75

                          90       100       110       120       130       140       150       160
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885   129 DvmrlmnvssSLNVSGvdsgvsfrnhtLTVQNLSFFNADYSSGYLY------GSLGLGGTLNSDTELEgdfinhsfFFLD 202
Cdd:pfam00026  76 D---------TVTVGG-----------LTITNQEFGLATKEPGSFFeyakfdGILGLGFPSISAVGAT--------PVFD 127

                         170       180       190       200       210       220       230       240
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885   203 ALKEARLINSSSYSLWLGSqkrngfadtsDANEAGYLIFGAVDPNLVEGEFRKFDMipyihpqtgkVAYGYPVVPMGPIY 282
Cdd:pfam00026 128 NLKSQGLIDSPAFSVYLNS----------PDAAGGEIIFGGVDPSKYTGSLTYVPV----------TSQGYWQITLDSVT 187

                         250       260       270       280       290       300       310       320
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885   283 ITSSSgrslNVTTDGFSApvLLDPSFALSYLPTKAIIQIAIQIAAVYVESlDLWLVSCDVASSGATVDFSFGDLTIKVPL 362
Cdd:pfam00026 188 VGGST----SACSSGCQA--ILDTGTSLLYGPTSIVSKIAKAVGASSSEY-GEYVVDCDSISTLPDITFVIGGAKITVPP 260

                         330       340       350       360       370       380
                  ....*....|....*....|....*....|....*....|....*....|....*....|....
gi 50284885   363 SDLlasthdqstntTLHFNTGQEACVLQLYPNTFTGYNVLGQAFMKNAYLAVDLEGKGVAMGQA 426
Cdd:pfam00026 261 SAY-----------VLQNSQGGSTCLSGFQPPPGGPLWILGDVFLRSAYVVFDRDNNRIGFAPA 313
gastricsin cd05477
Gastricsins, asparate proteases produced in gastric mucosa; Gastricsin is also called ...
 46-252 8.85e-04

Gastricsins, asparate proteases produced in gastric mucosa; Gastricsin is also called pepsinogen C. Gastricsins are produced in gastric mucosa of mammals. It is synthesized by the chief cells in the stomach as an inactive zymogen. It is self-converted to a mature enzyme under acidic conditions. Human gastricsin is distributed throughout all parts of the stomach. Gastricsin is synthesized as an inactive progastricsin that has an approximately 40 residue prosequence. It is self-converting to a mature enzyme being triggered by a drop in pH from neutrality to acidic conditions. Like other aspartic proteases, gastricsin are characterized by two catalytic aspartic residues at the active site, and display optimal activity at acidic pH. Mature enzyme has a pseudo-2-fold symmetry that passes through the active site between the catalytic aspartate residues. Structurally, aspartic proteases are bilobal enzymes, each lobe contributing a catalytic aspartate residue, with an extended active site cleft localized between the two lobes of the molecule. One lobe may be evolved from the other through ancient gene-duplication event. Although the three-dimensional structures of the two lobes are very similar, the amino acid sequences are more divergent, except for the conserved catalytic site motif. This family of aspartate proteases is classified by MEROPS as the peptidase family A1 (pepsin A, clan AA).


Pssm-ID: 133144 [Multi-domain]  Cd Length: 318  Bit Score: 41.80  E-value: 8.85e-04
                        10        20        30        40        50        60        70        80
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885  46 DGMYYVNATLGTPGQWQQLGLGLAQPYVWVVSGDADSQcnrldsGCLSGPLYYPQESRTSSTGGDKYSINFIDGiSLNGT 125
Cdd:cd05477   1 DMSYYGEISIGTPPQNFLVLFDTGSSNLWVPSVLCQSQ------ACTNHTKFNPSQSSTYSTNGETFSLQYGSG-SLTGI 73

                        90       100       110       120       130       140       150       160
                ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 50284885 126 RYMDVMRLMNVSsslnVSGVDSGVSfrnHTLTVQNLSFFNADYSSGYLYGSLGLGGTLNSdtelegdfinhsfffLDALK 205
Cdd:cd05477  74 FGYDTVTVQGII----ITNQEFGLS---ETEPGTNFVYAQFDGILGLAYPSISAGGATTV---------------MQGMM 131

                       170       180       190       200
                ....*....|....*....|....*....|....*....|....*..
gi 50284885 206 EARLINSSSYSLWLGSQKrngfadtsdANEAGYLIFGAVDPNLVEGE 252
Cdd:cd05477 132 QQNLLQAPIFSFYLSGQQ---------GQQGGELVFGGVDNNLYTGQ 169
 
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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