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Conserved domains on  [gi|1958667836|ref|XP_038944987|]
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nitric oxide synthase 1 isoform X1 [Rattus norvegicus]

Protein Classification

Graphical summary

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List of domain hits

Name Accession Description Interval E-value
NOS_oxygenase_euk cd00795
Nitric oxide synthase (NOS) eukaryotic oxygenase domain. NOS produces nitric oxide (NO) by ...
300-711 0e+00

Nitric oxide synthase (NOS) eukaryotic oxygenase domain. NOS produces nitric oxide (NO) by catalyzing a five-electron heme-based oxidation of a guanidine nitrogen of L-arginine to L-citrulline via two successive monooxygenation reactions producing N(omega)-hydroxy-L-arginine (NHA) as an intermediate. In mammals, there are three distinct NOS isozymes: neuronal (nNOS or NOS-1), cytokine-inducible (iNOS or NOS-2) and endothelial (eNOS or NOS-3) . Nitric oxide synthases are homodimers. In eukaryotes, each monomer has an N-terminal oxygenase domain, which binds to the substrate L-Arg, zinc, and to the cofactors heme and 5.6.7.8-(6R)-tetrahydrobiopterin (BH4) . Eukaryotic NOS's also have a C-terminal electron supplying reductase region, which is homologous to cytochrome P450 reductase and binds NADH, FAD and FMN.


:

Pssm-ID: 238410  Cd Length: 412  Bit Score: 927.09  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  300 FLKVKNWETDVVLTDTLHLKSTLETGCTEHICMGSIMLPSQHTRKPEDVRTKDQLFPLAKEFLDQYYSSIKRFGSKAHMD 379
Cdd:cd00795      1 FVRVKNWETGSILYDTLHSKATQDGPCTERRCLGSIMDPKKLTRRPRDGRPKEELLPQAKDFINQYYSSIKRSGSEAHLA 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  380 RLEEVNKEIESTSTYQLKDTELIYGAKHAWRNASRCVGRIQWSKLQVFDARDCTTAHGMFNYICNHVKYATNKGNLRSAI 459
Cdd:cd00795     81 RLEEVTKEIEATGTYQLTEDELIFGAKQAWRNAPRCIGRIQWSKLQVFDARDCTTAQEMFEAICNHIKYATNKGNLRSAI 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  460 TIFPQRTDGKHDFRVWNSQLIRYAGYKQPDGSTLGDPANVQFTEICIQQGWKAPRGRFDVLPLLLQANGNDPELFQIPPE 539
Cdd:cd00795    161 TVFPQRTDGKHDFRIWNSQLIRYAGYKQPDGSIIGDPANVEFTELCIKLGWKPKYGRFDVLPLVLQANGEDPELFEIPPE 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  540 LVLEVPIRHPKFDWFKDLGLKWYGLPAVSNMLLEIGGLEFSACPFSGWYMGTEIGVRDYCDNSRYNILEEVAKKMDLDMR 619
Cdd:cd00795    241 LVLEVPIEHPKYEWFKELGLKWYALPAVSNMLLEIGGLEFTACPFNGWYMGTEIGVRDLCDQQRYNILEEVAKKMGLDTR 320
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  620 KTSSLWKDQALVEINIAVLYSFQSDKVTIVDHHSATESFIKHMENEYRCRGGCPADWVWIVPPMSGSITPVFHQEMLNYR 699
Cdd:cd00795    321 KTSSLWKDKALVEINVAVLHSFQKANVTIVDHHSASESFMKHMENEYRARGGCPADWVWIVPPMSGSITPVFHQEMLNYV 400
                          410
                   ....*....|..
gi 1958667836  700 LTPSFEYQPDPW 711
Cdd:cd00795    401 LSPSYEYQPDPW 412
Nitric_oxide_synthase cd06202
The ferredoxin-reductase (FNR) like C-terminal domain of the nitric oxide synthase (NOS) fuses ...
1030-1433 0e+00

The ferredoxin-reductase (FNR) like C-terminal domain of the nitric oxide synthase (NOS) fuses with a heme-containing N-terminal oxidase domain. The reductase portion is similar in structure to NADPH dependent cytochrome-450 reductase (CYPOR), having an inserted connecting sub-domain within the FAD binding portion of FNR. NOS differs from CYPOR in a requirement for the cofactor tetrahydrobiopterin and unlike most CYPOR is dimeric. Nitric oxide synthase produces nitric oxide in the conversion of L-arginine to L-citruline. NOS has been implicated in a variety of processes including cytotoxicity, anti-inflamation, neurotransmission, and vascular smooth muscle relaxation.


:

Pssm-ID: 99799 [Multi-domain]  Cd Length: 406  Bit Score: 780.75  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1030 RLLSRQNLQSPKSSRSTIFVRLHTNGNQELQYQPGDHLGVFPGNHEDLVNALIERLEDAPPANHVVKVEMLEERNTALGV 1109
Cdd:cd06202      1 KVISRQNLQSPKSSRSTILVKLDTNGAQELHYQPGDHVGIFPANRPELVDALLDRLHDAPPPDQVIKLEVLEERSTALGI 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1110 ISNWKDESRLPPCTIFQAFKYYLDITTPPTPLQLQQFASLATNEKEKQRLLVLSKGLQEYEEWKWGKNPTMVEVLEEFPS 1189
Cdd:cd06202     81 IKTWTPHERLPPCTLRQALTRYLDITTPPTPQLLQLLATLATDEKDKERLEVLGKGSSEYEDWKWYKNPNILEVLEEFPS 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1190 IQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVHLTVAIVSYHTRDGEGPVHHGVCSSWLNRIQADDVVPCFVRGAPSFH 1269
Cdd:cd06202    161 LQVPASLLLTQLPLLQPRYYSISSSPDMYPGEIHLTVAVVSYRTRDGQGPVHHGVCSTWLNGLTPGDTVPCFVRSAPSFH 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1270 LPRNPQVPCILVGPGTGIAPFRSFWQQRQFDI---QHKGMNPCPMVLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAY 1346
Cdd:cd06202    241 LPEDPSVPVIMVGPGTGIAPFRSFWQQRQYDLrmsEDPGKKFGDMTLFFGCRNSTIDDIYKEETEEAKNKGVLTEVYTAL 320
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1347 SREPDRPKKYVQDVLQEQlAESVYRALKEQGGHIYVCGDVTMAADVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRYHE 1426
Cdd:cd06202    321 SREPGKPKTYVQDLLKEQ-AESVYDALVREGGHIYVCGDVTMAEDVSQTIQRILAEHGNMSAEEAEEFILKLRDENRYHE 399

                   ....*..
gi 1958667836 1427 DIFGVTL 1433
Cdd:cd06202    400 DIFGVTL 406
PDZ_nNOS-like cd06708
PDZ domain of neuronal nitric oxide synthase (nNOS), and related domains; PDZ (PSD-95 ...
14-123 4.78e-72

PDZ domain of neuronal nitric oxide synthase (nNOS), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of nNOS, and related domains. nNOS produces a key signaling molecule, nitric oxide (NO), which has diverse functions throughout the body and acts as a neurotransmitter and intracellular signaling molecule in the central and peripheral nervous system. nNOS is concentrated at synaptic junctions in the brain and motor endplates in skeletal muscle. The PDZ domain of neuronal nitric oxide synthase (nNOS) interacts with the PDZ domain of alpha1-syntrophin (in muscle cells) and with the second PDZ domain of Disks large homolog 4 (Dlg4, also known as PSD-95), and nitric oxide synthase 1 adaptor protein NOS1AP in neurons. Dlg4 binds NMDA receptors, and nNOS, forming a complex in neurons. NOS1AP competes with Dgl4 for the nNOS PDZ domain and prevents the coupling of nNos activation with NMDA receptor-mediated calcium influx. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This nNOS-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


:

Pssm-ID: 467192 [Multi-domain]  Cd Length: 110  Bit Score: 235.35  E-value: 4.78e-72
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   14 NVISVRLFKRKVGGLGFLVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHV 93
Cdd:cd06708      1 NVISVRLFKRKVGGLGFLVKQRVCKPPVIISDLIRGGAAEQSGLVQVGDIILAVNGRPLVDVSYESALEVLRSIPSETPV 80
                           90       100       110
                   ....*....|....*....|....*....|
gi 1958667836   94 VLILRGPEGFTTHLETTFTGDGTPKTIRVT 123
Cdd:cd06708     81 VLILRGPEGFTTHLETTFTGDGTPKTVRVT 110
Flavodoxin_1 pfam00258
Flavodoxin;
757-964 2.36e-29

Flavodoxin;


:

Pssm-ID: 425562 [Multi-domain]  Cd Length: 142  Bit Score: 114.77  E-value: 2.36e-29
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  757 ILYATETGKSQAYAKTLCEIFK-HAFDAKAMSMEEYDIV--HLEHEALVLVVTSTFGNGDPPENGEKFgCALMEMrhpns 833
Cdd:pfam00258    1 IFYGSQTGNTEKLAEAIAEGLGeAGFEVDVVDLDDVDETlsEIEEEDLLLVVVSTWGEGEPPDNAKPF-VDWLLL----- 74
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  834 vqeerkypeplrFFPRKGPSLShvdseahslvaardsqhrsykvrfnsvssysdsrkssgdgpdlrdnfestgplaNVRF 913
Cdd:pfam00258   75 ------------FGTLEDGDLS------------------------------------------------------GLKY 88
                          170       180       190       200       210
                   ....*....|....*....|....*....|....*....|....*....|....
gi 1958667836  914 SVFGLGSRAYPHFCAFGHAVDTLLEELGGERILKMREGDEL---CGQEEAFRTW 964
Cdd:pfam00258   89 AVFGLGDSGYEGFCGAAKKLDEKLSELGASRVGPLGEGDEDpqeDGLEEAFEAW 142
 
Name Accession Description Interval E-value
NOS_oxygenase_euk cd00795
Nitric oxide synthase (NOS) eukaryotic oxygenase domain. NOS produces nitric oxide (NO) by ...
300-711 0e+00

Nitric oxide synthase (NOS) eukaryotic oxygenase domain. NOS produces nitric oxide (NO) by catalyzing a five-electron heme-based oxidation of a guanidine nitrogen of L-arginine to L-citrulline via two successive monooxygenation reactions producing N(omega)-hydroxy-L-arginine (NHA) as an intermediate. In mammals, there are three distinct NOS isozymes: neuronal (nNOS or NOS-1), cytokine-inducible (iNOS or NOS-2) and endothelial (eNOS or NOS-3) . Nitric oxide synthases are homodimers. In eukaryotes, each monomer has an N-terminal oxygenase domain, which binds to the substrate L-Arg, zinc, and to the cofactors heme and 5.6.7.8-(6R)-tetrahydrobiopterin (BH4) . Eukaryotic NOS's also have a C-terminal electron supplying reductase region, which is homologous to cytochrome P450 reductase and binds NADH, FAD and FMN.


Pssm-ID: 238410  Cd Length: 412  Bit Score: 927.09  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  300 FLKVKNWETDVVLTDTLHLKSTLETGCTEHICMGSIMLPSQHTRKPEDVRTKDQLFPLAKEFLDQYYSSIKRFGSKAHMD 379
Cdd:cd00795      1 FVRVKNWETGSILYDTLHSKATQDGPCTERRCLGSIMDPKKLTRRPRDGRPKEELLPQAKDFINQYYSSIKRSGSEAHLA 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  380 RLEEVNKEIESTSTYQLKDTELIYGAKHAWRNASRCVGRIQWSKLQVFDARDCTTAHGMFNYICNHVKYATNKGNLRSAI 459
Cdd:cd00795     81 RLEEVTKEIEATGTYQLTEDELIFGAKQAWRNAPRCIGRIQWSKLQVFDARDCTTAQEMFEAICNHIKYATNKGNLRSAI 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  460 TIFPQRTDGKHDFRVWNSQLIRYAGYKQPDGSTLGDPANVQFTEICIQQGWKAPRGRFDVLPLLLQANGNDPELFQIPPE 539
Cdd:cd00795    161 TVFPQRTDGKHDFRIWNSQLIRYAGYKQPDGSIIGDPANVEFTELCIKLGWKPKYGRFDVLPLVLQANGEDPELFEIPPE 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  540 LVLEVPIRHPKFDWFKDLGLKWYGLPAVSNMLLEIGGLEFSACPFSGWYMGTEIGVRDYCDNSRYNILEEVAKKMDLDMR 619
Cdd:cd00795    241 LVLEVPIEHPKYEWFKELGLKWYALPAVSNMLLEIGGLEFTACPFNGWYMGTEIGVRDLCDQQRYNILEEVAKKMGLDTR 320
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  620 KTSSLWKDQALVEINIAVLYSFQSDKVTIVDHHSATESFIKHMENEYRCRGGCPADWVWIVPPMSGSITPVFHQEMLNYR 699
Cdd:cd00795    321 KTSSLWKDKALVEINVAVLHSFQKANVTIVDHHSASESFMKHMENEYRARGGCPADWVWIVPPMSGSITPVFHQEMLNYV 400
                          410
                   ....*....|..
gi 1958667836  700 LTPSFEYQPDPW 711
Cdd:cd00795    401 LSPSYEYQPDPW 412
Nitric_oxide_synthase cd06202
The ferredoxin-reductase (FNR) like C-terminal domain of the nitric oxide synthase (NOS) fuses ...
1030-1433 0e+00

The ferredoxin-reductase (FNR) like C-terminal domain of the nitric oxide synthase (NOS) fuses with a heme-containing N-terminal oxidase domain. The reductase portion is similar in structure to NADPH dependent cytochrome-450 reductase (CYPOR), having an inserted connecting sub-domain within the FAD binding portion of FNR. NOS differs from CYPOR in a requirement for the cofactor tetrahydrobiopterin and unlike most CYPOR is dimeric. Nitric oxide synthase produces nitric oxide in the conversion of L-arginine to L-citruline. NOS has been implicated in a variety of processes including cytotoxicity, anti-inflamation, neurotransmission, and vascular smooth muscle relaxation.


Pssm-ID: 99799 [Multi-domain]  Cd Length: 406  Bit Score: 780.75  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1030 RLLSRQNLQSPKSSRSTIFVRLHTNGNQELQYQPGDHLGVFPGNHEDLVNALIERLEDAPPANHVVKVEMLEERNTALGV 1109
Cdd:cd06202      1 KVISRQNLQSPKSSRSTILVKLDTNGAQELHYQPGDHVGIFPANRPELVDALLDRLHDAPPPDQVIKLEVLEERSTALGI 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1110 ISNWKDESRLPPCTIFQAFKYYLDITTPPTPLQLQQFASLATNEKEKQRLLVLSKGLQEYEEWKWGKNPTMVEVLEEFPS 1189
Cdd:cd06202     81 IKTWTPHERLPPCTLRQALTRYLDITTPPTPQLLQLLATLATDEKDKERLEVLGKGSSEYEDWKWYKNPNILEVLEEFPS 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1190 IQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVHLTVAIVSYHTRDGEGPVHHGVCSSWLNRIQADDVVPCFVRGAPSFH 1269
Cdd:cd06202    161 LQVPASLLLTQLPLLQPRYYSISSSPDMYPGEIHLTVAVVSYRTRDGQGPVHHGVCSTWLNGLTPGDTVPCFVRSAPSFH 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1270 LPRNPQVPCILVGPGTGIAPFRSFWQQRQFDI---QHKGMNPCPMVLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAY 1346
Cdd:cd06202    241 LPEDPSVPVIMVGPGTGIAPFRSFWQQRQYDLrmsEDPGKKFGDMTLFFGCRNSTIDDIYKEETEEAKNKGVLTEVYTAL 320
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1347 SREPDRPKKYVQDVLQEQlAESVYRALKEQGGHIYVCGDVTMAADVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRYHE 1426
Cdd:cd06202    321 SREPGKPKTYVQDLLKEQ-AESVYDALVREGGHIYVCGDVTMAEDVSQTIQRILAEHGNMSAEEAEEFILKLRDENRYHE 399

                   ....*..
gi 1958667836 1427 DIFGVTL 1433
Cdd:cd06202    400 DIFGVTL 406
NO_synthase pfam02898
Nitric oxide synthase, oxygenase domain;
350-711 0e+00

Nitric oxide synthase, oxygenase domain;


Pssm-ID: 460742  Cd Length: 362  Bit Score: 770.93  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  350 TKDQLFPLAKEFLDQYYSSIKRFgSKAHMDRLEEVNKEIESTSTYQLKDTELIYGAKHAWRNASRCVGRIQWSKLQVFDA 429
Cdd:pfam02898    1 PKEELLEEAKEFIEQYYTELKRS-SEEHEARWEEVRAEIEETGTYQHTYEELAYGAKLAWRNSNRCIGRIFWSKLQVFDA 79
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  430 RDCTTAHGMFNYICNHVKYATNKGNLRSAITIFPQRTDGKHDFRVWNSQLIRYAGYKQPDGSTLGDPANVQFTEICIQQG 509
Cdd:pfam02898   80 RHVTTEEEMFEALCNHIKYATNGGNIRSAITIFPPRTDGKHDFRIWNHQLIRYAGYEQPDGSVIGDPANVEFTELCEKLG 159
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  510 WKAPRGRFDVLPLLLQANGNDPELFQIPPELVLEVPIRHPKFDWFKDLGLKWYGLPAVSNMLLEIGGLEFSACPFSGWYM 589
Cdd:pfam02898  160 WKGKGTRFDVLPLVIQANGEDPKLFEIPPELVLEVPIEHPEYEWFAELGLKWYAVPAISNMRLEIGGIEYTAAPFNGWYM 239
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  590 GTEIGVRDYCDNSRYNILEEVAKKMDLDMRKTSSLWKDQALVEINIAVLYSFQSDKVTIVDHHSATESFIKHMENEYRCR 669
Cdd:pfam02898  240 GTEIGARNLADEYRYNLLEKVAKKMGLDTRSNSSLWKDRALVELNVAVLHSFQKAGVTIVDHHTAAEQFMKHEENEQRAG 319
                          330       340       350       360
                   ....*....|....*....|....*....|....*....|..
gi 1958667836  670 GGCPADWVWIVPPMSGSITPVFHQEMLNYRLTPSFEYQPDPW 711
Cdd:pfam02898  320 RGCPGDWVWLVPPLSGSTTPVFHQEMDNYILKPNFFYQEDPW 361
COG4362 COG4362
Nitric oxide synthase, oxygenase domain [Inorganic ion transport and metabolism];
358-709 0e+00

Nitric oxide synthase, oxygenase domain [Inorganic ion transport and metabolism];


Pssm-ID: 443495  Cd Length: 360  Bit Score: 575.66  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  358 AKEFLDQYYSSIKRFGSkAHMDRLEEVNKEIESTSTYQLKDTELIYGAKHAWRNASRCVGRIQWSKLQVFDARDCTTAHG 437
Cdd:COG4362     10 AEEFLRQCYKELGKSEE-EVERRLAEVRAEIAATGTYTHTYEELEYGARVAWRNSNRCIGRLFWRSLQVRDRRHVTTPEE 88
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  438 MFNYICNHVKYATNKGNLRSAITIFPQRTDGKHDFRVWNSQLIRYAGYKQPDGSTLGDPANVQFTEICIQQGWKAPRGRF 517
Cdd:COG4362     89 VFEALVEHLRFATNGGKIRPTITVFAPDQPGRPGVRIWNHQLIRYAGYETEDGSVLGDPASVEFTDACQRLGWRGPRTAF 168
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  518 DVLPLLLQANGNDPELFQIPPELVLEVPIRHPKFDWFKDLGLKWYGLPAVSNMLLEIGGLEFSACPFSGWYMGTEIGVRD 597
Cdd:COG4362    169 DVLPLVIQVGGEPPRLFEIPRDLVLEVPITHPEYPWFAELGLRWYAVPAISNMRLEIGGIDYPAAPFNGWYMGTEIGARN 248
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  598 YCDNSRYNILEEVAKKMDLDMRKTSSLWKDQALVEINIAVLYSFQSDKVTIVDHHSATESFIKHMENEYRCRGGCPADWV 677
Cdd:COG4362    249 LADEDRYNLLPKVAERMGLDTSSNRTLWKDRALVELNIAVLHSFKKAGVTIVDHHTASQQFLTFEQREEKAGREVTGDWS 328
                          330       340       350
                   ....*....|....*....|....*....|..
gi 1958667836  678 WIVPPMSGSITPVFHQEMLNYRLTPSFEYQPD 709
Cdd:COG4362    329 WLIPPMSGATTHVFHRYYDNEILKPNFFYQDD 360
CysJ COG0369
Flavoprotein (flavin reductase) subunit CysJ of sulfite and N-hydroxylaminopurine reductases ...
747-1429 3.13e-143

Flavoprotein (flavin reductase) subunit CysJ of sulfite and N-hydroxylaminopurine reductases [Nucleotide transport and metabolism, Inorganic ion transport and metabolism]; Flavoprotein (flavin reductase) subunit CysJ of sulfite and N-hydroxylaminopurine reductases is part of the Pathway/BioSystem: Cysteine biosynthesis


Pssm-ID: 440138 [Multi-domain]  Cd Length: 561  Bit Score: 451.14  E-value: 3.13e-143
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  747 QAMAKRVKATILYATETGKSQAYAKTLCEIFKHA-FDAKAMSMEEYDIVHLEHEALVLVVTSTFGNGDPPENGEKFGCAL 825
Cdd:COG0369     21 AAAAAGTPLTILYGSQTGNAEGLAEQLAERAKAAgLAVTLASLDDYKPKDLAKEGLLLIVTSTYGEGEPPDNARAFYEFL 100
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  826 MEMRHPNsvqeerkypeplrffprkgpslshvdseahslvaardsqhrsykvrfnsvssysdsrkssgdgpdlrdnfest 905
Cdd:COG0369    101 HSKKAPK------------------------------------------------------------------------- 107
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  906 gpLANVRFSVFGLGSRAYPHFCAFGHAVDTLLEELGGERILKMREGDElcGQEEAFRTWAKKVFKAACDVFcvgddvnie 985
Cdd:COG0369    108 --LDGLRYAVLGLGDSSYETFCQTGKDFDARLEELGATRLLPRVDCDV--DYEEAAEAWLAAVLAALAEAL--------- 174
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  986 KANNSLISNDrswkrnkfrltyVAEAPDLTqglsnvhKKRVSAARLLSRQNLQSPKSSRSTIFVRLHTnGNQELQYQPGD 1065
Cdd:COG0369    175 GAAAAAAAAA------------AAAAPAYS-------RKNPFPATVLENRELTGRGSAKETRHIEIDL-PGSGLSYEPGD 234
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1066 HLGVFPGNHEDLVNALIERLEDAPpaNHVVKVemleerntalgvisnwKDESRlppcTIFQAFKYYLDITTPPTPLqLQQ 1145
Cdd:COG0369    235 ALGVWPENDPALVDELLARLGLDG--DEPVTL----------------DGEPL----SLREALTEHLELTRLTPPL-LEK 291
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1146 FASLATNEKEKQrlLVLSKGLQEYEEWKWGKnpTMVEVLEEFPSIQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVHLT 1225
Cdd:COG0369    292 YAELTGNAELAA--LLADEDKAALREYLAGR--QLLDLLREFPAAELSAEELLELLRPLTPRLYSISSSPKAHPDEVHLT 367
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1226 VAIVSYHTrdgEGPVHHGVCSSWLNRIQADDVVPCFVRGAPSFHLPRNPQVPCILVGPGTGIAPFRSFWQQRQFDiQHKG 1305
Cdd:COG0369    368 VGVVRYEA---SGRERKGVASTYLADLEEGDTVPVFVEPNPNFRLPADPDTPIIMIGPGTGIAPFRAFLQEREAR-GASG 443
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1306 MNpcpmVLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAYSREpDRPKKYVQDVLQEQLAEsVYRALkEQGGHIYVCGD 1385
Cdd:COG0369    444 KN----WLFFGDRHFTTDFLYQTELQAWLKDGVLTRLDLAFSRD-QAEKIYVQHRLLEQGAE-LWAWL-EEGAHVYVCGD 516
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|....*
gi 1958667836 1386 VT-MAADVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRYHEDIF 1429
Cdd:COG0369    517 ASrMAKDVDAALLDIIAEHGGLSEEEAEEYLAELRAEKRYQRDVY 561
FAD_binding_1 pfam00667
FAD binding domain; This domain is found in sulfite reductase, NADPH cytochrome P450 reductase, ...
1020-1248 7.96e-92

FAD binding domain; This domain is found in sulfite reductase, NADPH cytochrome P450 reductase, Nitric oxide synthase and methionine synthase reductase.


Pssm-ID: 395540 [Multi-domain]  Cd Length: 219  Bit Score: 296.17  E-value: 7.96e-92
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1020 NVHKKRVSAARLLSRQNLQSPKSSRSTIFVRLHTNGnQELQYQPGDHLGVFPGNHEDLVNALIERLEDAPPANHVVKVEM 1099
Cdd:pfam00667    1 PFDAKKPFTAPVLSNRELTSPSSDRNCIHVELDISG-SGLTYQTGDHLGVYPPNNEELVEELLERLGLDPKPDTVVLLKT 79
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1100 LEErntalgvisnWKDESRLPPCTIFQAFKYYLDITTPPTPLQLQQFASLATNEKEKQRLLVLS--KGLQEYEEWKWGKN 1177
Cdd:pfam00667   80 LDE----------RVKPPRLPPTTYRQALKYYLDITGPPSKQLLRLLAQFAPEEEEKQRLEFLSsdAGAREYKRWKLNHA 149
                          170       180       190       200       210       220       230
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|.
gi 1958667836 1178 PTMVEVLEEFPSIQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVHLTVAIVSYHTrDGEGPVHHGVCSSW 1248
Cdd:pfam00667  150 PTLLEVLEEFPSVKLPADFLLTQLPQLQPRYYSISSSSKVHPNEVHLTVVVVEYET-DGEGRIHYGVCSNW 219
cysJ TIGR01931
sulfite reductase [NADPH] flavoprotein, alpha-component; This model describes an ...
756-1429 2.79e-81

sulfite reductase [NADPH] flavoprotein, alpha-component; This model describes an NADPH-dependent sulfite reductase flavoprotein subunit. Most members of this family are found in Cys biosynthesis gene clusters. The closest homologs below the trusted cutoff are designated as subunits nitrate reductase.


Pssm-ID: 273882 [Multi-domain]  Cd Length: 597  Bit Score: 280.43  E-value: 2.79e-81
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  756 TILYATETGKSQAYAKTLCEIFKHA-FDAKAMSMEEYDIVHLEHEALVLVVTSTFGNGDPPENGEKFGCALMEMRHPNsv 834
Cdd:TIGR01931   62 TILYGSQTGNARRLAKRLAEKLEAAgFSVRLSSADDYKFKQLKKERLLLLVISTQGEGEPPEEAISLHKFLHSKKAPK-- 139
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  835 qeerkypeplrffprkgpslshvdseahslvaardsqhrsykvrfnsvssysdsrkssgdgpdlrdnfestgpLANVRFS 914
Cdd:TIGR01931  140 -------------------------------------------------------------------------LENLRYS 146
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  915 VFGLGSRAYPHFCAFGHAVDTLLEELGGERILKMREGDelCGQEEAFRTWAKKVFKAACDVFCVG-DDVNIEKANNSLIS 993
Cdd:TIGR01931  147 VLGLGDSSYEFFCQTGKDFDKRLEELGGKRLLPRVDAD--LDYDANAAEWRAGVLTALNEQAKGGaSTPSASETSTPLQT 224
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  994 NDRSW-KRNKFRltyvaeapdltqglsnvhkkrvsaARLLSRQNLQSPKSSRSTIFVRLHTnGNQELQYQPGDHLGVFPG 1072
Cdd:TIGR01931  225 STSVYsKQNPFR------------------------AEVLENQKITGRNSKKDVRHIEIDL-EGSGLHYEPGDALGVWYK 279
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1073 NHEDLVNALIERLEDAPPANHVVKVEMLeerntalgvisnwkdesrlppcTIFQAFKYYLDITTPPTPLqLQQFASLATN 1152
Cdd:TIGR01931  280 NDPALVKEILKLLNLDPDEKVTIGGKTI----------------------PLFEALITHFELTQNTKPL-LKAYAELTGN 336
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1153 EkEKQRLLVLSKGLQEYEEwkwgkNPTMVEVLEEFPSiQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVHLTVAIVSYh 1232
Cdd:TIGR01931  337 K-ELKALIADNEKLKAYIQ-----NTPLIDLIRDYPA-DLDAEQLISLLRPLTPRLYSISSSQSEVGDEVHLTVGVVRY- 408
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1233 trDGEGPVHHGVCSSWL-NRIQADDVVPCFVRGAPSFHLPRNPQVPCILVGPGTGIAPFRSFWQQRQfDIQHKGMNpcpm 1311
Cdd:TIGR01931  409 --QAHGRARLGGASGFLaERLKEGDTVPVYIEPNDNFRLPEDPDTPIIMIGPGTGVAPFRAFMQERA-EDGAKGKN---- 481
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1312 VLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAYSREpDRPKKYVQDVLQEQLAEsVYRALkEQGGHIYVCGDVT-MAA 1390
Cdd:TIGR01931  482 WLFFGNPHFTTDFLYQVEWQNYLKKGVLTKMDLAFSRD-QAEKIYVQHRIREQGAE-LWQWL-QEGAHIYVCGDAKkMAK 558
                          650       660       670
                   ....*....|....*....|....*....|....*....
gi 1958667836 1391 DVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRYHEDIF 1429
Cdd:TIGR01931  559 DVHQALLDIIAKEGHLDAEEAEEYLTDLRVEKRYQRDVY 597
PDZ_nNOS-like cd06708
PDZ domain of neuronal nitric oxide synthase (nNOS), and related domains; PDZ (PSD-95 ...
14-123 4.78e-72

PDZ domain of neuronal nitric oxide synthase (nNOS), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of nNOS, and related domains. nNOS produces a key signaling molecule, nitric oxide (NO), which has diverse functions throughout the body and acts as a neurotransmitter and intracellular signaling molecule in the central and peripheral nervous system. nNOS is concentrated at synaptic junctions in the brain and motor endplates in skeletal muscle. The PDZ domain of neuronal nitric oxide synthase (nNOS) interacts with the PDZ domain of alpha1-syntrophin (in muscle cells) and with the second PDZ domain of Disks large homolog 4 (Dlg4, also known as PSD-95), and nitric oxide synthase 1 adaptor protein NOS1AP in neurons. Dlg4 binds NMDA receptors, and nNOS, forming a complex in neurons. NOS1AP competes with Dgl4 for the nNOS PDZ domain and prevents the coupling of nNos activation with NMDA receptor-mediated calcium influx. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This nNOS-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467192 [Multi-domain]  Cd Length: 110  Bit Score: 235.35  E-value: 4.78e-72
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   14 NVISVRLFKRKVGGLGFLVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHV 93
Cdd:cd06708      1 NVISVRLFKRKVGGLGFLVKQRVCKPPVIISDLIRGGAAEQSGLVQVGDIILAVNGRPLVDVSYESALEVLRSIPSETPV 80
                           90       100       110
                   ....*....|....*....|....*....|
gi 1958667836   94 VLILRGPEGFTTHLETTFTGDGTPKTIRVT 123
Cdd:cd06708     81 VLILRGPEGFTTHLETTFTGDGTPKTVRVT 110
cysJ PRK10953
NADPH-dependent assimilatory sulfite reductase flavoprotein subunit;
756-1429 4.69e-66

NADPH-dependent assimilatory sulfite reductase flavoprotein subunit;


Pssm-ID: 182862 [Multi-domain]  Cd Length: 600  Bit Score: 235.77  E-value: 4.69e-66
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  756 TILYATETGKsqayAKTLCEIFKHAFDAKAMSME-----EYDIVHLEHEALVLVVTSTFGNGDPPENGekfgCALmemrh 830
Cdd:PRK10953    65 TLISASQTGN----ARRVAEQLRDDLLAAKLNVNlvnagDYKFKQIAQEKLLIVVTSTQGEGEPPEEA----VAL----- 131
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  831 pnsvqeeRKYpeplrFFPRKGPSLShvdseahslvaardsqhrsykvrfnsvssysdsrkssgdgpdlrdnfestgplaN 910
Cdd:PRK10953   132 -------HKF-----LFSKKAPKLE------------------------------------------------------N 145
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  911 VRFSVFGLGSRAYPHFCAFGHAVDTLLEELGGERILKMREGD-ELCGQEEAFRTWAKKVFKAACDVFCVGDDVNIEKANN 989
Cdd:PRK10953   146 TAFAVFGLGDTSYEFFCQAGKDFDSKLAELGAERLLDRVDADvEYQAAASEWRARVVDALKSRAPAVAAPSQSVATGAVN 225
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  990 SLISNdrswkrnkfrlTYVAEAPdLTQGLSnVHKKrvsaarLLSRQnlqSPKSSRStIFVRLhtnGNQELQYQPGDHLGV 1069
Cdd:PRK10953   226 EIHTS-----------PYSKEAP-LTASLS-VNQK------ITGRN---SEKDVRH-IEIDL---GDSGLRYQPGDALGV 279
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1070 FPGNHEDLVNALIERL---EDAPpanhvVKVemleerntalgvisnwkDESRLPpctIFQAFKYYLDITTPpTPLQLQQF 1146
Cdd:PRK10953   280 WYQNDPALVKELVELLwlkGDEP-----VTV-----------------DGKTLP---LAEALQWHFELTVN-TANIVENY 333
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1147 ASLATNEKekqrLLVL---SKGLQEYeewkwGKNPTMVEVLEEFPSiQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVH 1223
Cdd:PRK10953   334 ATLTRSET----LLPLvgdKAALQHY-----AATTPIVDMVRFAPA-QLDAEQLIGLLRPLTPRLYSIASSQAEVENEVH 403
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1224 LTVAIVSYhtrDGEGPVHHGVCSSWL-NRIQADDVVPCFVRGAPSFHLPRNPQVPCILVGPGTGIAPFRSFWQQRQFDiQ 1302
Cdd:PRK10953   404 ITVGVVRY---DIEGRARAGGASSFLaDRLEEEGEVRVFIEHNDNFRLPANPETPVIMIGPGTGIAPFRAFMQQRAAD-G 479
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1303 HKGMNpcpmVLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAYSRepDRPKK-YVQDVLQEQLAEsVYRALkEQGGHIY 1381
Cdd:PRK10953   480 APGKN----WLFFGNPHFTEDFLYQVEWQRYVKEGLLTRIDLAWSR--DQKEKiYVQDKLREQGAE-LWRWI-NDGAHIY 551
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|....*....
gi 1958667836 1382 VCGDVT-MAADVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRYHEDIF 1429
Cdd:PRK10953   552 VCGDANrMAKDVEQALLEVIAEFGGMDTEAADEFLSELRVERRYQRDVY 600
Flavodoxin_1 pfam00258
Flavodoxin;
757-964 2.36e-29

Flavodoxin;


Pssm-ID: 425562 [Multi-domain]  Cd Length: 142  Bit Score: 114.77  E-value: 2.36e-29
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  757 ILYATETGKSQAYAKTLCEIFK-HAFDAKAMSMEEYDIV--HLEHEALVLVVTSTFGNGDPPENGEKFgCALMEMrhpns 833
Cdd:pfam00258    1 IFYGSQTGNTEKLAEAIAEGLGeAGFEVDVVDLDDVDETlsEIEEEDLLLVVVSTWGEGEPPDNAKPF-VDWLLL----- 74
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  834 vqeerkypeplrFFPRKGPSLShvdseahslvaardsqhrsykvrfnsvssysdsrkssgdgpdlrdnfestgplaNVRF 913
Cdd:pfam00258   75 ------------FGTLEDGDLS------------------------------------------------------GLKY 88
                          170       180       190       200       210
                   ....*....|....*....|....*....|....*....|....*....|....
gi 1958667836  914 SVFGLGSRAYPHFCAFGHAVDTLLEELGGERILKMREGDEL---CGQEEAFRTW 964
Cdd:pfam00258   89 AVFGLGDSGYEGFCGAAKKLDEKLSELGASRVGPLGEGDEDpqeDGLEEAFEAW 142
PDZ pfam00595
PDZ domain; PDZ domains are found in diverse signaling proteins.
17-96 1.72e-16

PDZ domain; PDZ domains are found in diverse signaling proteins.


Pssm-ID: 395476 [Multi-domain]  Cd Length: 81  Bit Score: 75.78  E-value: 1.72e-16
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   17 SVRLFKRKVGGLGFLVKERVSK--PPVIISDLIRGGAAEQSGlIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVV 94
Cdd:pfam00595    1 QVTLEKDGRGGLGFSLKGGSDQgdPGIFVSEVLPGGAAEAGG-LKVGDRILSINGQDVENMTHEEAVLALKGSGGKVTLT 79

                   ..
gi 1958667836   95 LI 96
Cdd:pfam00595   80 IL 81
PDZ smart00228
Domain present in PSD-95, Dlg, and ZO-1/2; Also called DHR (Dlg homologous region) or GLGF ...
14-100 5.54e-14

Domain present in PSD-95, Dlg, and ZO-1/2; Also called DHR (Dlg homologous region) or GLGF (relatively well conserved tetrapeptide in these domains). Some PDZs have been shown to bind C-terminal polypeptides; others appear to bind internal (non-C-terminal) polypeptides. Different PDZs possess different binding specificities.


Pssm-ID: 214570 [Multi-domain]  Cd Length: 85  Bit Score: 68.56  E-value: 5.54e-14
                            10        20        30        40        50        60        70        80
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836    14 NVISVRLFKRKvGGLGF-LVKERVSKPPVIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVDLSYDSALEVLRGiASETH 92
Cdd:smart00228    1 EPRLVELEKGG-GGLGFsLVGGKDEGGGVVVSSVVPGSPAAKAGL-RVGDVILEVNGTSVEGLTHLEAVDLLKK-AGGKV 77

                    ....*...
gi 1958667836    93 VVLILRGP 100
Cdd:smart00228   78 TLTVLRGG 85
CtpA COG0793
C-terminal processing protease CtpA/Prc, contains a PDZ domain [Posttranslational modification, ...
22-123 3.65e-10

C-terminal processing protease CtpA/Prc, contains a PDZ domain [Posttranslational modification, protein turnover, chaperones];


Pssm-ID: 440556 [Multi-domain]  Cd Length: 341  Bit Score: 63.35  E-value: 3.65e-10
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   22 KRKVGGLGFLVKERvsKPPVIISDLIRGGAAEQSGlIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVVLILRGpe 101
Cdd:COG0793     56 SGEFGGLGAELGEE--DGKVVVVSVIPGSPAEKAG-IKPGDIILAIDGKSVAGLTLDDAVKLLRGKAGTKVTLTIKRP-- 130
                           90       100
                   ....*....|....*....|..
gi 1958667836  102 gftthlettftGDGTPKTIRVT 123
Cdd:COG0793    131 -----------GEGEPITVTLT 141
PRK08105 PRK08105
flavodoxin; Provisional
893-952 2.38e-08

flavodoxin; Provisional


Pssm-ID: 181230 [Multi-domain]  Cd Length: 149  Bit Score: 54.51  E-value: 2.38e-08
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*...
gi 1958667836  893 GDGPD--------LRDNFestGPLANVRFSVFGLGSRAYPHFCAFGHAVDTLLEELGGERILKMREGD 952
Cdd:PRK08105    62 GDLPDsivplfqaLKDTA---GYQPNLRYGVIALGDSSYDNFCGAGKQFDALLQEQGAKRVGERLEID 126
FldA COG0716
Flavodoxin [Energy production and conversion]; Flavodoxin is part of the Pathway/BioSystem: ...
755-821 1.08e-03

Flavodoxin [Energy production and conversion]; Flavodoxin is part of the Pathway/BioSystem: Heme biosynthesis


Pssm-ID: 440480 [Multi-domain]  Cd Length: 135  Bit Score: 40.66  E-value: 1.08e-03
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1958667836  755 ATILYATETGKSQAYAKTLCEIFKhAFDAKAMSMEEYDIVHLEHEALVLVVTSTFGnGDPPENGEKF 821
Cdd:COG0716      1 ILIVYGSTTGNTEKVAEAIAEALG-AAGVDLFEIEDADLDDLEDYDLLILGTPTWA-GELPDDWEDF 65
degP_htrA_DO TIGR02037
periplasmic serine protease, Do/DeqQ family; This family consists of a set proteins various ...
41-155 2.91e-03

periplasmic serine protease, Do/DeqQ family; This family consists of a set proteins various designated DegP, heat shock protein HtrA, and protease DO. The ortholog in Pseudomonas aeruginosa is designated MucD and is found in an operon that controls mucoid phenotype. This family also includes the DegQ (HhoA) paralog in E. coli which can rescue a DegP mutant, but not the smaller DegS paralog, which cannot. Members of this family are located in the periplasm and have separable functions as both protease and chaperone. Members have a trypsin domain and two copies of a PDZ domain. This protein protects bacteria from thermal and other stresses and may be important for the survival of bacterial pathogens.// The chaperone function is dominant at low temperatures, whereas the proteolytic activity is turned on at elevated temperatures. [Protein fate, Protein folding and stabilization, Protein fate, Degradation of proteins, peptides, and glycopeptides]


Pssm-ID: 273938 [Multi-domain]  Cd Length: 428  Bit Score: 41.82  E-value: 2.91e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   41 VIISDLIRGGAAEQSGLiQAGDIILAVNDRPLvdlsyDSALEVLRGIAS----ETHVVLILRgpegftthlettftgDGT 116
Cdd:TIGR02037  259 ALVAQVLPGSPAEKAGL-KAGDVITSVNGKPI-----SSFADLRRAIGTlkpgKKVTLGILR---------------KGK 317
                           90       100       110
                   ....*....|....*....|....*....|....*....
gi 1958667836  117 PKTIRVTqplgpptkavdLSHQPSASKDQSLAVDRVTGL 155
Cdd:TIGR02037  318 EKTITVT-----------LGASPEEQASSSNPFLGLTVA 345
 
Name Accession Description Interval E-value
NOS_oxygenase_euk cd00795
Nitric oxide synthase (NOS) eukaryotic oxygenase domain. NOS produces nitric oxide (NO) by ...
300-711 0e+00

Nitric oxide synthase (NOS) eukaryotic oxygenase domain. NOS produces nitric oxide (NO) by catalyzing a five-electron heme-based oxidation of a guanidine nitrogen of L-arginine to L-citrulline via two successive monooxygenation reactions producing N(omega)-hydroxy-L-arginine (NHA) as an intermediate. In mammals, there are three distinct NOS isozymes: neuronal (nNOS or NOS-1), cytokine-inducible (iNOS or NOS-2) and endothelial (eNOS or NOS-3) . Nitric oxide synthases are homodimers. In eukaryotes, each monomer has an N-terminal oxygenase domain, which binds to the substrate L-Arg, zinc, and to the cofactors heme and 5.6.7.8-(6R)-tetrahydrobiopterin (BH4) . Eukaryotic NOS's also have a C-terminal electron supplying reductase region, which is homologous to cytochrome P450 reductase and binds NADH, FAD and FMN.


Pssm-ID: 238410  Cd Length: 412  Bit Score: 927.09  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  300 FLKVKNWETDVVLTDTLHLKSTLETGCTEHICMGSIMLPSQHTRKPEDVRTKDQLFPLAKEFLDQYYSSIKRFGSKAHMD 379
Cdd:cd00795      1 FVRVKNWETGSILYDTLHSKATQDGPCTERRCLGSIMDPKKLTRRPRDGRPKEELLPQAKDFINQYYSSIKRSGSEAHLA 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  380 RLEEVNKEIESTSTYQLKDTELIYGAKHAWRNASRCVGRIQWSKLQVFDARDCTTAHGMFNYICNHVKYATNKGNLRSAI 459
Cdd:cd00795     81 RLEEVTKEIEATGTYQLTEDELIFGAKQAWRNAPRCIGRIQWSKLQVFDARDCTTAQEMFEAICNHIKYATNKGNLRSAI 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  460 TIFPQRTDGKHDFRVWNSQLIRYAGYKQPDGSTLGDPANVQFTEICIQQGWKAPRGRFDVLPLLLQANGNDPELFQIPPE 539
Cdd:cd00795    161 TVFPQRTDGKHDFRIWNSQLIRYAGYKQPDGSIIGDPANVEFTELCIKLGWKPKYGRFDVLPLVLQANGEDPELFEIPPE 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  540 LVLEVPIRHPKFDWFKDLGLKWYGLPAVSNMLLEIGGLEFSACPFSGWYMGTEIGVRDYCDNSRYNILEEVAKKMDLDMR 619
Cdd:cd00795    241 LVLEVPIEHPKYEWFKELGLKWYALPAVSNMLLEIGGLEFTACPFNGWYMGTEIGVRDLCDQQRYNILEEVAKKMGLDTR 320
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  620 KTSSLWKDQALVEINIAVLYSFQSDKVTIVDHHSATESFIKHMENEYRCRGGCPADWVWIVPPMSGSITPVFHQEMLNYR 699
Cdd:cd00795    321 KTSSLWKDKALVEINVAVLHSFQKANVTIVDHHSASESFMKHMENEYRARGGCPADWVWIVPPMSGSITPVFHQEMLNYV 400
                          410
                   ....*....|..
gi 1958667836  700 LTPSFEYQPDPW 711
Cdd:cd00795    401 LSPSYEYQPDPW 412
NOS_oxygenase cd00575
Nitric oxide synthase (NOS) produces nitric oxide (NO) by catalyzing a five-electron ...
353-708 0e+00

Nitric oxide synthase (NOS) produces nitric oxide (NO) by catalyzing a five-electron heme-based oxidation of a guanidine nitrogen of L-arginine to L-citrulline via two successive monooxygenation reactions producing N(omega)-hydroxy-L-arginine (NHA) as an intermediate. In mammals, there are three distinct NOS isozymes: neuronal (nNOS or NOS-1), cytokine-inducible (iNOS or NOS-2) and endothelial (eNOS or NOS-3) . Nitric oxide synthases are homodimers. In eukaryotes, each monomer has an N-terminal oxygenase domain which binds to the substrate L-Arg, zinc, and to the cofactors heme and 5.6.7.8-(6R)-tetrahydrobiopterin (BH4) . Eukaryotic NOSs also have a C-terminal electron supplying reductase region, which is homologous to cytochrome P450 reductase and binds NADH, FAD and FMN. While prokaryotes can produce NO as a byproduct of denitrification, using a completely different set of enzymes than NOS, a few prokaryotes also have a NOS which consists solely of the NOS oxygenase domain. Prokaryotic NOS binds to the substrate L-Arg, zinc, and to the cofactors heme and tetrahydrofolate.


Pssm-ID: 238321  Cd Length: 356  Bit Score: 787.24  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  353 QLFPLAKEFLDQYYSSIKRFGSKAHMDRLEEVNKEIESTSTYQLKDTELIYGAKHAWRNASRCVGRIQWSKLQVFDARDC 432
Cdd:cd00575      1 ELLPQAKDFINQYYSSIKRSGSEAHEARLEEVEKEIEATGTYQLTEEELIYGAKMAWRNAPRCIGRIQWSKLQVFDARDV 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  433 TTAHGMFNYICNHVKYATNKGNLRSAITIFPQRTDGKHDFRVWNSQLIRYAGYKQPDGSTLGDPANVQFTEICIQQGWKA 512
Cdd:cd00575     81 TTAQEMFEAICNHIKYATNGGNIRSAITVFPQRTDGKHDFRIWNSQLIRYAGYKQPDGSIIGDPANVEFTELCIQLGWKP 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  513 PRGRFDVLPLLLQANGNDPELFQIPPELVLEVPIRHPKFDWFKDLGLKWYGLPAVSNMLLEIGGLEFSACPFSGWYMGTE 592
Cdd:cd00575    161 KGGRFDVLPLVLQANGEDPELFEIPPELVLEVPIEHPKYEWFAELGLKWYALPAVSNMLLEIGGLEFPAAPFNGWYMGTE 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  593 IGVRDYCDNSRYNILEEVAKKMDLDMRKTSSLWKDQALVEINIAVLYSFQSDKVTIVDHHSATESFIKHMENEYRCRGGC 672
Cdd:cd00575    241 IGVRNLCDTQRYNILEKVARKMGLDTRKNSSLWKDRALVELNVAVLHSFQKAGVTIVDHHTAAESFMKHLENEYRARGGC 320
                          330       340       350
                   ....*....|....*....|....*....|....*.
gi 1958667836  673 PADWVWIVPPMSGSITPVFHQEMLNYRLTPSFEYQP 708
Cdd:cd00575    321 PADWVWLVPPMSGSLTPVFHQEMLNYVLSPSFFYQP 356
Nitric_oxide_synthase cd06202
The ferredoxin-reductase (FNR) like C-terminal domain of the nitric oxide synthase (NOS) fuses ...
1030-1433 0e+00

The ferredoxin-reductase (FNR) like C-terminal domain of the nitric oxide synthase (NOS) fuses with a heme-containing N-terminal oxidase domain. The reductase portion is similar in structure to NADPH dependent cytochrome-450 reductase (CYPOR), having an inserted connecting sub-domain within the FAD binding portion of FNR. NOS differs from CYPOR in a requirement for the cofactor tetrahydrobiopterin and unlike most CYPOR is dimeric. Nitric oxide synthase produces nitric oxide in the conversion of L-arginine to L-citruline. NOS has been implicated in a variety of processes including cytotoxicity, anti-inflamation, neurotransmission, and vascular smooth muscle relaxation.


Pssm-ID: 99799 [Multi-domain]  Cd Length: 406  Bit Score: 780.75  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1030 RLLSRQNLQSPKSSRSTIFVRLHTNGNQELQYQPGDHLGVFPGNHEDLVNALIERLEDAPPANHVVKVEMLEERNTALGV 1109
Cdd:cd06202      1 KVISRQNLQSPKSSRSTILVKLDTNGAQELHYQPGDHVGIFPANRPELVDALLDRLHDAPPPDQVIKLEVLEERSTALGI 80
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1110 ISNWKDESRLPPCTIFQAFKYYLDITTPPTPLQLQQFASLATNEKEKQRLLVLSKGLQEYEEWKWGKNPTMVEVLEEFPS 1189
Cdd:cd06202     81 IKTWTPHERLPPCTLRQALTRYLDITTPPTPQLLQLLATLATDEKDKERLEVLGKGSSEYEDWKWYKNPNILEVLEEFPS 160
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1190 IQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVHLTVAIVSYHTRDGEGPVHHGVCSSWLNRIQADDVVPCFVRGAPSFH 1269
Cdd:cd06202    161 LQVPASLLLTQLPLLQPRYYSISSSPDMYPGEIHLTVAVVSYRTRDGQGPVHHGVCSTWLNGLTPGDTVPCFVRSAPSFH 240
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1270 LPRNPQVPCILVGPGTGIAPFRSFWQQRQFDI---QHKGMNPCPMVLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAY 1346
Cdd:cd06202    241 LPEDPSVPVIMVGPGTGIAPFRSFWQQRQYDLrmsEDPGKKFGDMTLFFGCRNSTIDDIYKEETEEAKNKGVLTEVYTAL 320
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1347 SREPDRPKKYVQDVLQEQlAESVYRALKEQGGHIYVCGDVTMAADVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRYHE 1426
Cdd:cd06202    321 SREPGKPKTYVQDLLKEQ-AESVYDALVREGGHIYVCGDVTMAEDVSQTIQRILAEHGNMSAEEAEEFILKLRDENRYHE 399

                   ....*..
gi 1958667836 1427 DIFGVTL 1433
Cdd:cd06202    400 DIFGVTL 406
NO_synthase pfam02898
Nitric oxide synthase, oxygenase domain;
350-711 0e+00

Nitric oxide synthase, oxygenase domain;


Pssm-ID: 460742  Cd Length: 362  Bit Score: 770.93  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  350 TKDQLFPLAKEFLDQYYSSIKRFgSKAHMDRLEEVNKEIESTSTYQLKDTELIYGAKHAWRNASRCVGRIQWSKLQVFDA 429
Cdd:pfam02898    1 PKEELLEEAKEFIEQYYTELKRS-SEEHEARWEEVRAEIEETGTYQHTYEELAYGAKLAWRNSNRCIGRIFWSKLQVFDA 79
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  430 RDCTTAHGMFNYICNHVKYATNKGNLRSAITIFPQRTDGKHDFRVWNSQLIRYAGYKQPDGSTLGDPANVQFTEICIQQG 509
Cdd:pfam02898   80 RHVTTEEEMFEALCNHIKYATNGGNIRSAITIFPPRTDGKHDFRIWNHQLIRYAGYEQPDGSVIGDPANVEFTELCEKLG 159
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  510 WKAPRGRFDVLPLLLQANGNDPELFQIPPELVLEVPIRHPKFDWFKDLGLKWYGLPAVSNMLLEIGGLEFSACPFSGWYM 589
Cdd:pfam02898  160 WKGKGTRFDVLPLVIQANGEDPKLFEIPPELVLEVPIEHPEYEWFAELGLKWYAVPAISNMRLEIGGIEYTAAPFNGWYM 239
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  590 GTEIGVRDYCDNSRYNILEEVAKKMDLDMRKTSSLWKDQALVEINIAVLYSFQSDKVTIVDHHSATESFIKHMENEYRCR 669
Cdd:pfam02898  240 GTEIGARNLADEYRYNLLEKVAKKMGLDTRSNSSLWKDRALVELNVAVLHSFQKAGVTIVDHHTAAEQFMKHEENEQRAG 319
                          330       340       350       360
                   ....*....|....*....|....*....|....*....|..
gi 1958667836  670 GGCPADWVWIVPPMSGSITPVFHQEMLNYRLTPSFEYQPDPW 711
Cdd:pfam02898  320 RGCPGDWVWLVPPLSGSTTPVFHQEMDNYILKPNFFYQEDPW 361
COG4362 COG4362
Nitric oxide synthase, oxygenase domain [Inorganic ion transport and metabolism];
358-709 0e+00

Nitric oxide synthase, oxygenase domain [Inorganic ion transport and metabolism];


Pssm-ID: 443495  Cd Length: 360  Bit Score: 575.66  E-value: 0e+00
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  358 AKEFLDQYYSSIKRFGSkAHMDRLEEVNKEIESTSTYQLKDTELIYGAKHAWRNASRCVGRIQWSKLQVFDARDCTTAHG 437
Cdd:COG4362     10 AEEFLRQCYKELGKSEE-EVERRLAEVRAEIAATGTYTHTYEELEYGARVAWRNSNRCIGRLFWRSLQVRDRRHVTTPEE 88
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  438 MFNYICNHVKYATNKGNLRSAITIFPQRTDGKHDFRVWNSQLIRYAGYKQPDGSTLGDPANVQFTEICIQQGWKAPRGRF 517
Cdd:COG4362     89 VFEALVEHLRFATNGGKIRPTITVFAPDQPGRPGVRIWNHQLIRYAGYETEDGSVLGDPASVEFTDACQRLGWRGPRTAF 168
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  518 DVLPLLLQANGNDPELFQIPPELVLEVPIRHPKFDWFKDLGLKWYGLPAVSNMLLEIGGLEFSACPFSGWYMGTEIGVRD 597
Cdd:COG4362    169 DVLPLVIQVGGEPPRLFEIPRDLVLEVPITHPEYPWFAELGLRWYAVPAISNMRLEIGGIDYPAAPFNGWYMGTEIGARN 248
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  598 YCDNSRYNILEEVAKKMDLDMRKTSSLWKDQALVEINIAVLYSFQSDKVTIVDHHSATESFIKHMENEYRCRGGCPADWV 677
Cdd:COG4362    249 LADEDRYNLLPKVAERMGLDTSSNRTLWKDRALVELNIAVLHSFKKAGVTIVDHHTASQQFLTFEQREEKAGREVTGDWS 328
                          330       340       350
                   ....*....|....*....|....*....|..
gi 1958667836  678 WIVPPMSGSITPVFHQEMLNYRLTPSFEYQPD 709
Cdd:COG4362    329 WLIPPMSGATTHVFHRYYDNEILKPNFFYQDD 360
NOS_oxygenase_prok cd00794
Nitric oxide synthase (NOS) prokaryotic oxygenase domain. NOS produces nitric oxide (NO) by ...
354-708 5.84e-146

Nitric oxide synthase (NOS) prokaryotic oxygenase domain. NOS produces nitric oxide (NO) by catalyzing a five-electron heme-based oxidation of a guanidine nitrogen of L-arginine to L-citrulline via two successive monooxygenation reactions producing N(omega)-hydroxy-L-arginine (NHA) as an intermediate. Nitric oxide synthases are homodimers. Most prokaryotes produce NO as a byproduct of denitrification, using a completely different set of enzymes than NOS. However, a few prokaryotes also have a NOS, consisting solely of the NOS oxygenase domain. Prokaryotic NOS binds to the substrate L-Arg, zinc, and to the cofactors heme and tetrahydrofolate.


Pssm-ID: 238409  Cd Length: 353  Bit Score: 450.35  E-value: 5.84e-146
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  354 LFPLAKEFLDQYYSSIKRFGSKAhmDRLEEVNKEIESTSTYQLKDTELIYGAKHAWRNASRCVGRIQWSKLQVFDARDCT 433
Cdd:cd00794      2 LFKEARAFLTNMYEELGETGELN--KRLAAVESEIDETGTYTHTTEELVYGAKMAWRNSNRCIGRLFWESLNVRDARDVR 79
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  434 TAHGMFNYICNHVKYATNKGNLRSAITIFPQRTDGKHDFRVWNSQLIRYAGYKQPDGSTlGDPANVQFTEICIQQGWKAP 513
Cdd:cd00794     80 TEEEVAEALLDHITEATNGGKIRPYITIFAPEAPGKDGPRIWNNQLIRYAGYERPGANI-GDPASAKFTRLAERLGWKGK 158
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  514 RGRFDVLPLLLQANGNDPELFQIPPELVLEVPIRHPKFDWFKDLGLKWYGLPAVSNMLLEIGGLEFSACPFSGWYMGTEI 593
Cdd:cd00794    159 GTNFDVLPLIIQLPGDRPKWFELPNDAVKEVPITHPHYPKIRKLGLKWYAVPIISDMDLEIGGIHYPAAPFNGWYMGTEI 238
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  594 GVRDYCDNSRYNILEEVAKKMDLDMRKTSSLWKDQALVEINIAVLYSFQSDKVTIVDHHSATESFIKHMENEYRCRGGCP 673
Cdd:cd00794    239 GARNLADEYRYNLLPKVAEALGLDTLKNRSLWKDRALVELNVAVLHSFKKAGVSIVDHHTAAKQFERFEEREARAGRKVT 318
                          330       340       350
                   ....*....|....*....|....*....|....*
gi 1958667836  674 ADWVWIVPPMSGSITPVFHQEMLNYRLTPSFEYQP 708
Cdd:cd00794    319 GKWSWLIPPLSPATTHIFHRGYDNTEVHPNFFYQK 353
CysJ COG0369
Flavoprotein (flavin reductase) subunit CysJ of sulfite and N-hydroxylaminopurine reductases ...
747-1429 3.13e-143

Flavoprotein (flavin reductase) subunit CysJ of sulfite and N-hydroxylaminopurine reductases [Nucleotide transport and metabolism, Inorganic ion transport and metabolism]; Flavoprotein (flavin reductase) subunit CysJ of sulfite and N-hydroxylaminopurine reductases is part of the Pathway/BioSystem: Cysteine biosynthesis


Pssm-ID: 440138 [Multi-domain]  Cd Length: 561  Bit Score: 451.14  E-value: 3.13e-143
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  747 QAMAKRVKATILYATETGKSQAYAKTLCEIFKHA-FDAKAMSMEEYDIVHLEHEALVLVVTSTFGNGDPPENGEKFGCAL 825
Cdd:COG0369     21 AAAAAGTPLTILYGSQTGNAEGLAEQLAERAKAAgLAVTLASLDDYKPKDLAKEGLLLIVTSTYGEGEPPDNARAFYEFL 100
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  826 MEMRHPNsvqeerkypeplrffprkgpslshvdseahslvaardsqhrsykvrfnsvssysdsrkssgdgpdlrdnfest 905
Cdd:COG0369    101 HSKKAPK------------------------------------------------------------------------- 107
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  906 gpLANVRFSVFGLGSRAYPHFCAFGHAVDTLLEELGGERILKMREGDElcGQEEAFRTWAKKVFKAACDVFcvgddvnie 985
Cdd:COG0369    108 --LDGLRYAVLGLGDSSYETFCQTGKDFDARLEELGATRLLPRVDCDV--DYEEAAEAWLAAVLAALAEAL--------- 174
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  986 KANNSLISNDrswkrnkfrltyVAEAPDLTqglsnvhKKRVSAARLLSRQNLQSPKSSRSTIFVRLHTnGNQELQYQPGD 1065
Cdd:COG0369    175 GAAAAAAAAA------------AAAAPAYS-------RKNPFPATVLENRELTGRGSAKETRHIEIDL-PGSGLSYEPGD 234
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1066 HLGVFPGNHEDLVNALIERLEDAPpaNHVVKVemleerntalgvisnwKDESRlppcTIFQAFKYYLDITTPPTPLqLQQ 1145
Cdd:COG0369    235 ALGVWPENDPALVDELLARLGLDG--DEPVTL----------------DGEPL----SLREALTEHLELTRLTPPL-LEK 291
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1146 FASLATNEKEKQrlLVLSKGLQEYEEWKWGKnpTMVEVLEEFPSIQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVHLT 1225
Cdd:COG0369    292 YAELTGNAELAA--LLADEDKAALREYLAGR--QLLDLLREFPAAELSAEELLELLRPLTPRLYSISSSPKAHPDEVHLT 367
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1226 VAIVSYHTrdgEGPVHHGVCSSWLNRIQADDVVPCFVRGAPSFHLPRNPQVPCILVGPGTGIAPFRSFWQQRQFDiQHKG 1305
Cdd:COG0369    368 VGVVRYEA---SGRERKGVASTYLADLEEGDTVPVFVEPNPNFRLPADPDTPIIMIGPGTGIAPFRAFLQEREAR-GASG 443
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1306 MNpcpmVLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAYSREpDRPKKYVQDVLQEQLAEsVYRALkEQGGHIYVCGD 1385
Cdd:COG0369    444 KN----WLFFGDRHFTTDFLYQTELQAWLKDGVLTRLDLAFSRD-QAEKIYVQHRLLEQGAE-LWAWL-EEGAHVYVCGD 516
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|....*
gi 1958667836 1386 VT-MAADVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRYHEDIF 1429
Cdd:COG0369    517 ASrMAKDVDAALLDIIAEHGGLSEEEAEEYLAELRAEKRYQRDVY 561
CYPOR_like cd06182
NADPH cytochrome p450 reductase (CYPOR) serves as an electron donor in several oxygenase ...
1030-1429 9.22e-105

NADPH cytochrome p450 reductase (CYPOR) serves as an electron donor in several oxygenase systems and is a component of nitric oxide synthases and methionine synthase reductases. CYPOR transfers two electrons from NADPH to the heme of cytochrome p450 via FAD and FMN. CYPOR has a C-terminal ferredoxin reducatase (FNR)- like FAD and NAD binding module, an FMN-binding domain, and an additional conecting domain (inserted within the FAD binding region) that orients the FNR and FMN binding domains. Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria and participate in a wide variety of redox metabolic pathways. The C-terminal domain contains most of the NADP(H) binding residues and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule which lies largely in a large gap betweed the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2, which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99779 [Multi-domain]  Cd Length: 267  Bit Score: 334.69  E-value: 9.22e-105
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1030 RLLSRQNLQSPKSSRSTIFVRLHTNGNQELQYQPGDHLGVFPGNhedlvnalierledappanhvvkvemleerntalgv 1109
Cdd:cd06182      1 AITVNRKLTPPDSPRSTRHLEFDLSGNSVLKYQPGDHLGVIPPN------------------------------------ 44
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1110 isnwkdesrlppctifqafkyyldittpptPLQlqqfaslatnekekqrllvlskglqeyeewkwgknptmvevleefps 1189
Cdd:cd06182     45 ------------------------------PLQ----------------------------------------------- 47
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1190 iqmpatllltqlsllqPRYYSISSSPDMYPDEVHLTVAIVSYHtrDGEGPVHHGVCSSWLNRIQADDVVPCFVRGAPSFH 1269
Cdd:cd06182     48 ----------------PRYYSIASSPDVDPGEVHLCVRVVSYE--APAGRIRKGVCSNFLAGLQLGAKVTVFIRPAPSFR 109
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1270 LPRNPQVPCILVGPGTGIAPFRSFWQQRQFDiQHKGMNPCPMVLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAYSRE 1349
Cdd:cd06182    110 LPKDPTTPIIMVGPGTGIAPFRGFLQERAAL-RANGKARGPAWLFFGCRNFASDYLYREELQEALKDGALTRLDVAFSRE 188
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1350 PDRPKKYVQDVLQEQlAESVYRALKEqGGHIYVCGDVT-MAADVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRYHEDI 1428
Cdd:cd06182    189 QAEPKVYVQDKLKEH-AEELRRLLNE-GAHIYVCGDAKsMAKDVEDALVKIIAKAGGVDESDAEEYLKELEDEGRYVEDV 266

                   .
gi 1958667836 1429 F 1429
Cdd:cd06182    267 W 267
CYPOR cd06204
NADPH cytochrome p450 reductase (CYPOR) serves as an electron donor in several oxygenase ...
1042-1428 9.78e-101

NADPH cytochrome p450 reductase (CYPOR) serves as an electron donor in several oxygenase systems and is a component of nitric oxide synthases and methionine synthase reductases. CYPOR transfers two electrons from NADPH to the heme of cytochrome p450 via FAD and FMN. Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria in which they participate in a wide variety of redox metabolic pathways. The C-terminal domain contains most of the NADP(H) binding residues and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule which lies largely in a large gap betweed the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2 which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99801 [Multi-domain]  Cd Length: 416  Bit Score: 329.60  E-value: 9.78e-101
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1042 SSRSTIFVRLHTnGNQELQYQPGDHLGVFPGNHEDLVNALIERLeDAPPANHVVKVEMLEERNTALGVIsnwkdesrLPP 1121
Cdd:cd06204     20 SDRSCLHIEFDI-SGSGIRYQTGDHLAVWPTNPSEEVERLLKVL-GLDDRDTVISLKSLDEPASKKVPF--------PCP 89
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1122 CTIFQAFKYYLDITTPPTPLQLQQFASLATNEKEKQRLLVL-SKGLQEYEewKWGKNP--TMVEVLEEFPSIQ---MPAT 1195
Cdd:cd06204     90 TTYRTALRHYLDITAPVSRQVLAALAQFAPDPEEKERLLKLaSEGKDEYA--KWIVEPhrNLLEVLQDFPSAKptpPPFD 167
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1196 LLLTQLSLLQPRYYSISSSPDMYPDEVHLTVAIVSYHTrdGEGPVHHGVCSSWLNRIQADDV------------------ 1257
Cdd:cd06204    168 FLIELLPRLQPRYYSISSSSKVHPNRIHITAVVVKYPT--PTGRIIKGVATNWLLALKPALNgekpptpyylsgprkkgg 245
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1258 ---VPCFVRGApSFHLPRNPQVPCILVGPGTGIAPFRSFWQQRQFdIQHKGMNPCPMVLVFGCRQSKIDHIYREETLQAK 1334
Cdd:cd06204    246 gskVPVFVRRS-NFRLPTKPSTPVIMIGPGTGVAPFRGFIQERAA-LKESGKKVGPTLLFFGCRHPDEDFIYKDELEEYA 323
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1335 NKGVFRELYTAYSREPDRpKKYVQDVLQEQlAESVYRALKEqGGHIYVCGDV-TMAADVLKAIQRIMTQQGKLSEEDAGV 1413
Cdd:cd06204    324 KLGGLLELVTAFSREQPK-KVYVQHRLAEH-AEQVWELINE-GAYIYVCGDAkNMARDVEKTLLEILAEQGGMTETEAEE 400
                          410
                   ....*....|....*
gi 1958667836 1414 FISRLRDDNRYHEDI 1428
Cdd:cd06204    401 YVKKLKTRGRYQEDV 415
FAD_binding_1 pfam00667
FAD binding domain; This domain is found in sulfite reductase, NADPH cytochrome P450 reductase, ...
1020-1248 7.96e-92

FAD binding domain; This domain is found in sulfite reductase, NADPH cytochrome P450 reductase, Nitric oxide synthase and methionine synthase reductase.


Pssm-ID: 395540 [Multi-domain]  Cd Length: 219  Bit Score: 296.17  E-value: 7.96e-92
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1020 NVHKKRVSAARLLSRQNLQSPKSSRSTIFVRLHTNGnQELQYQPGDHLGVFPGNHEDLVNALIERLEDAPPANHVVKVEM 1099
Cdd:pfam00667    1 PFDAKKPFTAPVLSNRELTSPSSDRNCIHVELDISG-SGLTYQTGDHLGVYPPNNEELVEELLERLGLDPKPDTVVLLKT 79
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1100 LEErntalgvisnWKDESRLPPCTIFQAFKYYLDITTPPTPLQLQQFASLATNEKEKQRLLVLS--KGLQEYEEWKWGKN 1177
Cdd:pfam00667   80 LDE----------RVKPPRLPPTTYRQALKYYLDITGPPSKQLLRLLAQFAPEEEEKQRLEFLSsdAGAREYKRWKLNHA 149
                          170       180       190       200       210       220       230
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|.
gi 1958667836 1178 PTMVEVLEEFPSIQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVHLTVAIVSYHTrDGEGPVHHGVCSSW 1248
Cdd:pfam00667  150 PTLLEVLEEFPSVKLPADFLLTQLPQLQPRYYSISSSSKVHPNEVHLTVVVVEYET-DGEGRIHYGVCSNW 219
CyPoR_like cd06207
NADPH cytochrome p450 reductase (CYPOR) serves as an electron donor in several oxygenase ...
1037-1424 1.37e-86

NADPH cytochrome p450 reductase (CYPOR) serves as an electron donor in several oxygenase systems and is a component of nitric oxide synthases and methionine synthase reductases. CYPOR transfers two electrons from NADPH to the heme of cytochrome p450 via FAD and FMN. Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria in which they participate in a wide variety of redox metabolic pathways. The C-terminal domain contains most of the NADP(H) binding residues and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule which lies largely in a large gap betweed the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2 which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99803 [Multi-domain]  Cd Length: 382  Bit Score: 288.02  E-value: 1.37e-86
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1037 LQSPKSSRSTIFVRLHTnGNQELQYQPGDHLGVFPGNHEDLVNALIERL-EDAppaNHVVKVEMLEERNTALGVISnwkd 1115
Cdd:cd06207      8 LTPADYDRSTRHIEFDL-GGSGLSYETGDNLGIYPENSDALVDEFLARLgLDG---DDVVRVEPNEQQRGKPPFPE---- 79
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1116 esrlpPCTIFQAFKYYLDITTPPTPLQLQQFASLATNEKEKQRLLVLS--KGLQEYEEWKWGknpTMVEVLEEFPSIQMP 1193
Cdd:cd06207     80 -----PISVRQLLKKFLDIFGKPTKKFLKLLSQLATDEEEKEDLYKLAsrEGRTEYKRYEKY---TYLEVLKDFPSVRPT 151
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1194 ATLLLTQLSLLQPRYYSISSSPDMYPDEVHLTVAIVSYHTRDGEgpVHHGVCSSWLNRIQADDVVPCFVRgAPSFHLPRN 1273
Cdd:cd06207    152 LEQLLELCPLIKPRYYSISSSPLKNPNEVHLLVSLVSWKTPSGR--SRYGLCSSYLAGLKVGQRVTVFIK-KSSFKLPKD 228
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1274 PQVPCILVGPGTGIAPFRSFWQQRQFDIQhKGMNPCPMVLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAYSREPDRp 1353
Cdd:cd06207    229 PKKPIIMVGPGTGLAPFRAFLQERAALLA-QGPEIGPVLLYFGCRHEDKDYLYKEELEEYEKSGVLTTLGTAFSRDQPK- 306
                          330       340       350       360       370       380       390
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|..
gi 1958667836 1354 KKYVQDVLQEQLAEsVYRALKEQGGHIYVCGDVT-MAADVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRY 1424
Cdd:cd06207    307 KVYVQDLIRENSDL-VYQLLEEGAGVIYVCGSTWkMPPDVQEAFEEILKKHGGGDEELAEKKIEELEERGRY 377
SiR cd06199
Cytochrome p450- like alpha subunits of E. coli sulfite reductase (SiR) multimerize with beta ...
1030-1429 8.88e-84

Cytochrome p450- like alpha subunits of E. coli sulfite reductase (SiR) multimerize with beta subunits to catalyze the NADPH dependent reduction of sulfite to sulfide. Beta subunits have an Fe4S4 cluster and a siroheme, while the alpha subunits (cysJ gene) are of the cytochrome p450 (CyPor) family having FAD and FMN as prosthetic groups and utilizing NADPH. Cypor (including cyt -450 reductase, nitric oxide synthase, and methionine synthase reductase) are ferredoxin reductase (FNR)-like proteins with an additional N-terminal FMN domain and a connecting sub-domain inserted within the flavin binding portion of the FNR-like domain. The connecting domain orients the N-terminal FMN domain with the C-terminal FNR domain.


Pssm-ID: 99796 [Multi-domain]  Cd Length: 360  Bit Score: 279.11  E-value: 8.88e-84
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1030 RLLSRQNLQSPKSSRSTIFVRLHTNGNQeLQYQPGDHLGVFPGNHEDLVNALIERLEdAPPANHVVKVEMLEErntalgv 1109
Cdd:cd06199      1 TVLENRLLTGPGSEKETRHIELDLEGSG-LSYEPGDALGVYPTNDPALVDELLAALG-LSGDEPVSTVGGGTL------- 71
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1110 isnwkdesrlppcTIFQAFKYYLDITTPPTPLqlqqFASLATNEKEKQRLLvlSKGLQEYEEWKWGKnptmvEVLEEFP- 1188
Cdd:cd06199     72 -------------PLREALIKHYEITTLLLAL----LESYAADTGALELLA--LAALEAVLAFAELR-----DVLDLLPi 127
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1189 -SIQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVHLTVAIVSYHTRDGEgpvHHGVCSSWL-NRIQADDVVPCFVRGAP 1266
Cdd:cd06199    128 pPARLTAEELLDLLRPLQPRLYSIASSPKAVPDEVHLTVAVVRYESHGRE---RKGVASTFLaDRLKEGDTVPVFVQPNP 204
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1267 SFHLPRNPQVPCILVGPGTGIAPFRSFWQQRQFDiQHKGMNpcpmVLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAY 1346
Cdd:cd06199    205 HFRLPEDPDAPIIMVGPGTGIAPFRAFLQEREAT-GAKGKN----WLFFGERHFATDFLYQDELQQWLKDGVLTRLDTAF 279
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1347 SRepDRPKK-YVQDVLQEQLAEsVYRALkEQGGHIYVCGDVT-MAADVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRY 1424
Cdd:cd06199    280 SR--DQAEKvYVQDRMREQGAE-LWAWL-EEGAHFYVCGDAKrMAKDVDAALLDIIATEGGMDEEEAEAYLKELKKEKRY 355

                   ....*
gi 1958667836 1425 HEDIF 1429
Cdd:cd06199    356 QRDVY 360
cysJ TIGR01931
sulfite reductase [NADPH] flavoprotein, alpha-component; This model describes an ...
756-1429 2.79e-81

sulfite reductase [NADPH] flavoprotein, alpha-component; This model describes an NADPH-dependent sulfite reductase flavoprotein subunit. Most members of this family are found in Cys biosynthesis gene clusters. The closest homologs below the trusted cutoff are designated as subunits nitrate reductase.


Pssm-ID: 273882 [Multi-domain]  Cd Length: 597  Bit Score: 280.43  E-value: 2.79e-81
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  756 TILYATETGKSQAYAKTLCEIFKHA-FDAKAMSMEEYDIVHLEHEALVLVVTSTFGNGDPPENGEKFGCALMEMRHPNsv 834
Cdd:TIGR01931   62 TILYGSQTGNARRLAKRLAEKLEAAgFSVRLSSADDYKFKQLKKERLLLLVISTQGEGEPPEEAISLHKFLHSKKAPK-- 139
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  835 qeerkypeplrffprkgpslshvdseahslvaardsqhrsykvrfnsvssysdsrkssgdgpdlrdnfestgpLANVRFS 914
Cdd:TIGR01931  140 -------------------------------------------------------------------------LENLRYS 146
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  915 VFGLGSRAYPHFCAFGHAVDTLLEELGGERILKMREGDelCGQEEAFRTWAKKVFKAACDVFCVG-DDVNIEKANNSLIS 993
Cdd:TIGR01931  147 VLGLGDSSYEFFCQTGKDFDKRLEELGGKRLLPRVDAD--LDYDANAAEWRAGVLTALNEQAKGGaSTPSASETSTPLQT 224
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  994 NDRSW-KRNKFRltyvaeapdltqglsnvhkkrvsaARLLSRQNLQSPKSSRSTIFVRLHTnGNQELQYQPGDHLGVFPG 1072
Cdd:TIGR01931  225 STSVYsKQNPFR------------------------AEVLENQKITGRNSKKDVRHIEIDL-EGSGLHYEPGDALGVWYK 279
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1073 NHEDLVNALIERLEDAPPANHVVKVEMLeerntalgvisnwkdesrlppcTIFQAFKYYLDITTPPTPLqLQQFASLATN 1152
Cdd:TIGR01931  280 NDPALVKEILKLLNLDPDEKVTIGGKTI----------------------PLFEALITHFELTQNTKPL-LKAYAELTGN 336
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1153 EkEKQRLLVLSKGLQEYEEwkwgkNPTMVEVLEEFPSiQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVHLTVAIVSYh 1232
Cdd:TIGR01931  337 K-ELKALIADNEKLKAYIQ-----NTPLIDLIRDYPA-DLDAEQLISLLRPLTPRLYSISSSQSEVGDEVHLTVGVVRY- 408
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1233 trDGEGPVHHGVCSSWL-NRIQADDVVPCFVRGAPSFHLPRNPQVPCILVGPGTGIAPFRSFWQQRQfDIQHKGMNpcpm 1311
Cdd:TIGR01931  409 --QAHGRARLGGASGFLaERLKEGDTVPVYIEPNDNFRLPEDPDTPIIMIGPGTGVAPFRAFMQERA-EDGAKGKN---- 481
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1312 VLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAYSREpDRPKKYVQDVLQEQLAEsVYRALkEQGGHIYVCGDVT-MAA 1390
Cdd:TIGR01931  482 WLFFGNPHFTTDFLYQVEWQNYLKKGVLTKMDLAFSRD-QAEKIYVQHRIREQGAE-LWQWL-QEGAHIYVCGDAKkMAK 558
                          650       660       670
                   ....*....|....*....|....*....|....*....
gi 1958667836 1391 DVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRYHEDIF 1429
Cdd:TIGR01931  559 DVHQALLDIIAKEGHLDAEEAEEYLTDLRVEKRYQRDVY 597
bifunctional_CYPOR cd06206
These bifunctional proteins fuse N-terminal cytochrome p450 with a cytochrome p450 reductase ...
1025-1429 9.33e-78

These bifunctional proteins fuse N-terminal cytochrome p450 with a cytochrome p450 reductase (CYPOR). NADPH cytochrome p450 reductase serves as an electron donor in several oxygenase systems and is a component of nitric oxide synthases and methionine synthase reductases. CYPOR transfers two electrons from NADPH to the heme of cytochrome p450 via FAD and FMN. Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria in which they participate in a wide variety of redox metabolic pathways. The C-terminal domain contains most of the NADP(H) binding residues and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule which lies largely in a large gap betweed the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2 which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99802 [Multi-domain]  Cd Length: 384  Bit Score: 262.97  E-value: 9.33e-78
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1025 RVSAARLLSrqnlqSPKSSRST--IFVRLHTNGNqelqYQPGDHLGVFPGNHEDLVNALIERLEDAPPAnhVVKVEMlEE 1102
Cdd:cd06206      1 TVVENRELT-----APGVGPSKrhLELRLPDGMT----YRAGDYLAVLPRNPPELVRRALRRFGLAWDT--VLTISA-SG 68
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1103 RNTAL--GVisnwkdesrlpPCTIFQAFKYYLDITTPPTPLQLQQFASLATNEKEKQRLLVLSKglQEYEEWKWGKNPTM 1180
Cdd:cd06206     69 SATGLplGT-----------PISVSELLSSYVELSQPATRRQLAALAEATRCPDTKALLERLAG--EAYAAEVLAKRVSV 135
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1181 VEVLEEFPSIQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVHLTVAIVSYHTRDGEGPvHHGVCSSWLNRIQADDVVPC 1260
Cdd:cd06206    136 LDLLERFPSIALPLATFLAMLPPMRPRQYSISSSPLVDPGHATLTVSVLDAPALSGQGR-YRGVASSYLSSLRPGDSIHV 214
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1261 FVRGA-PSFHLPRNPQVPCILVGPGTGIAPFRSFWQQRQFDIQHkGMNPCPMVLVFGCRQSKIDHIYREETLQAKNKGVF 1339
Cdd:cd06206    215 SVRPShSAFRPPSDPSTPLIMIAAGTGLAPFRGFLQERAALLAQ-GRKLAPALLFFGCRHPDHDDLYRDELEEWEAAGVV 293
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1340 rELYTAYSREPDRPKKYVQDVLQEQLAESVyrALKEQGGHIYVCGDVTMAADVLKAIQRIMTQQGKL----SEEDAGVFI 1415
Cdd:cd06206    294 -SVRRAYSRPPGGGCRYVQDRLWAEREEVW--ELWEQGARVYVCGDGRMAPGVREVLKRIYAEKDERgggsDDEEAEEWL 370
                          410
                   ....*....|....
gi 1958667836 1416 SRLRDDNRYHEDIF 1429
Cdd:cd06206    371 EELRNKGRYATDVF 384
PDZ_nNOS-like cd06708
PDZ domain of neuronal nitric oxide synthase (nNOS), and related domains; PDZ (PSD-95 ...
14-123 4.78e-72

PDZ domain of neuronal nitric oxide synthase (nNOS), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of nNOS, and related domains. nNOS produces a key signaling molecule, nitric oxide (NO), which has diverse functions throughout the body and acts as a neurotransmitter and intracellular signaling molecule in the central and peripheral nervous system. nNOS is concentrated at synaptic junctions in the brain and motor endplates in skeletal muscle. The PDZ domain of neuronal nitric oxide synthase (nNOS) interacts with the PDZ domain of alpha1-syntrophin (in muscle cells) and with the second PDZ domain of Disks large homolog 4 (Dlg4, also known as PSD-95), and nitric oxide synthase 1 adaptor protein NOS1AP in neurons. Dlg4 binds NMDA receptors, and nNOS, forming a complex in neurons. NOS1AP competes with Dgl4 for the nNOS PDZ domain and prevents the coupling of nNos activation with NMDA receptor-mediated calcium influx. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This nNOS-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467192 [Multi-domain]  Cd Length: 110  Bit Score: 235.35  E-value: 4.78e-72
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   14 NVISVRLFKRKVGGLGFLVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHV 93
Cdd:cd06708      1 NVISVRLFKRKVGGLGFLVKQRVCKPPVIISDLIRGGAAEQSGLVQVGDIILAVNGRPLVDVSYESALEVLRSIPSETPV 80
                           90       100       110
                   ....*....|....*....|....*....|
gi 1958667836   94 VLILRGPEGFTTHLETTFTGDGTPKTIRVT 123
Cdd:cd06708     81 VLILRGPEGFTTHLETTFTGDGTPKTVRVT 110
methionine_synthase_red cd06203
Human methionine synthase reductase (MSR) restores methionine sythase which is responsible for ...
1055-1428 8.51e-70

Human methionine synthase reductase (MSR) restores methionine sythase which is responsible for the regeneration of methionine from homocysteine, as well as the coversion of methyltetrahydrofolate to tetrahydrofolate. In MSR, electrons are transferred from NADPH to FAD to FMN to cob(II)alamin. MSR resembles proteins of the cytochrome p450 family including nitric oxide synthase, the alpha subunit of sulfite reductase, but contains an extended hinge region. NADPH cytochrome p450 reductase (CYPOR) serves as an electron donor in several oxygenase systems and is a component of nitric oxide synthases and methionine synthase reductases. CYPOR transfers two electrons from NADPH to the heme of cytochrome p450 via FAD and FMN. CYPORs resemble ferredoxin reductase (FNR) but have a connecting subdomain inserted within the flavin binding region, which helps orient the FMN binding doamin with the FNR module. Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria in which they participate in a wide variety of redox metabolic pathways. The C-terminal domain contains most of the NADP(H) binding residues and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule which lies largely in a large gap betweed the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2 which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99800 [Multi-domain]  Cd Length: 398  Bit Score: 240.30  E-value: 8.51e-70
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1055 GNQELQYQPGDHLGVFPGNHEDLVNALIERLEDAPPANHVVKVEMLeeRNTAlgvisnwKDESRLPP-----CTIFQAFK 1129
Cdd:cd06203     25 SPTGFDYQPGDTIGILPPNTASEVESLLKRLGLLEQADQPCEVKVV--PNTK-------KKNAKVPVhipkvVTLRTILT 95
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1130 YYLDITTPPTPLQLQQFASLATNEKEKQRLLVLS--KGLQEYEEWKWGKNPTMVEVLEEFPSIQMPATLLLTQLSLLQPR 1207
Cdd:cd06203     96 WCLDIRAIPKKPLLRALAEFTSDDNEKRRLEELCskQGSEDYTDFVRKRGLSLLDLLEAFPSCRPPLSLLIEHLPRLQPR 175
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1208 YYSISSSPDMYPDEVHLTVAIVSYhtrdgegpVHHGVCSSWLNRIQAD-----DVVPCFVRGAPSFHLP-RNPQVPCILV 1281
Cdd:cd06203    176 PYSIASSPLEGPGKLRFIFSVVEF--------PAKGLCTSWLESLCLSasshgVKVPFYLRSSSRFRLPpDDLRRPIIMV 247
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1282 GPGTGIAPFRSFWQQRQFDIQHKGMNPC-PMVLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAYSREPD--RPKKYVQ 1358
Cdd:cd06203    248 GPGTGVAPFLGFLQHREKLKESHTETVFgEAWLFFGCRHRDRDYLFRDELEEFLEEGILTRLIVAFSRDENdgSTPKYVQ 327
                          330       340       350       360       370       380       390
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|.
gi 1958667836 1359 DVLQEQlAESVYRALKEQGGHIYVCGDV-TMAADVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRYHEDI 1428
Cdd:cd06203    328 DKLEER-GKKLVDLLLNSNAKIYVCGDAkGMAKDVRDTFVDILSKELGLDKLEAKKLLARLRKEDRYLEDV 397
cysJ PRK10953
NADPH-dependent assimilatory sulfite reductase flavoprotein subunit;
756-1429 4.69e-66

NADPH-dependent assimilatory sulfite reductase flavoprotein subunit;


Pssm-ID: 182862 [Multi-domain]  Cd Length: 600  Bit Score: 235.77  E-value: 4.69e-66
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  756 TILYATETGKsqayAKTLCEIFKHAFDAKAMSME-----EYDIVHLEHEALVLVVTSTFGNGDPPENGekfgCALmemrh 830
Cdd:PRK10953    65 TLISASQTGN----ARRVAEQLRDDLLAAKLNVNlvnagDYKFKQIAQEKLLIVVTSTQGEGEPPEEA----VAL----- 131
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  831 pnsvqeeRKYpeplrFFPRKGPSLShvdseahslvaardsqhrsykvrfnsvssysdsrkssgdgpdlrdnfestgplaN 910
Cdd:PRK10953   132 -------HKF-----LFSKKAPKLE------------------------------------------------------N 145
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  911 VRFSVFGLGSRAYPHFCAFGHAVDTLLEELGGERILKMREGD-ELCGQEEAFRTWAKKVFKAACDVFCVGDDVNIEKANN 989
Cdd:PRK10953   146 TAFAVFGLGDTSYEFFCQAGKDFDSKLAELGAERLLDRVDADvEYQAAASEWRARVVDALKSRAPAVAAPSQSVATGAVN 225
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  990 SLISNdrswkrnkfrlTYVAEAPdLTQGLSnVHKKrvsaarLLSRQnlqSPKSSRStIFVRLhtnGNQELQYQPGDHLGV 1069
Cdd:PRK10953   226 EIHTS-----------PYSKEAP-LTASLS-VNQK------ITGRN---SEKDVRH-IEIDL---GDSGLRYQPGDALGV 279
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1070 FPGNHEDLVNALIERL---EDAPpanhvVKVemleerntalgvisnwkDESRLPpctIFQAFKYYLDITTPpTPLQLQQF 1146
Cdd:PRK10953   280 WYQNDPALVKELVELLwlkGDEP-----VTV-----------------DGKTLP---LAEALQWHFELTVN-TANIVENY 333
                          410       420       430       440       450       460       470       480
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1147 ASLATNEKekqrLLVL---SKGLQEYeewkwGKNPTMVEVLEEFPSiQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVH 1223
Cdd:PRK10953   334 ATLTRSET----LLPLvgdKAALQHY-----AATTPIVDMVRFAPA-QLDAEQLIGLLRPLTPRLYSIASSQAEVENEVH 403
                          490       500       510       520       530       540       550       560
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1224 LTVAIVSYhtrDGEGPVHHGVCSSWL-NRIQADDVVPCFVRGAPSFHLPRNPQVPCILVGPGTGIAPFRSFWQQRQFDiQ 1302
Cdd:PRK10953   404 ITVGVVRY---DIEGRARAGGASSFLaDRLEEEGEVRVFIEHNDNFRLPANPETPVIMIGPGTGIAPFRAFMQQRAAD-G 479
                          570       580       590       600       610       620       630       640
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1303 HKGMNpcpmVLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAYSRepDRPKK-YVQDVLQEQLAEsVYRALkEQGGHIY 1381
Cdd:PRK10953   480 APGKN----WLFFGNPHFTEDFLYQVEWQRYVKEGLLTRIDLAWSR--DQKEKiYVQDKLREQGAE-LWRWI-NDGAHIY 551
                          650       660       670       680
                   ....*....|....*....|....*....|....*....|....*....
gi 1958667836 1382 VCGDVT-MAADVLKAIQRIMTQQGKLSEEDAGVFISRLRDDNRYHEDIF 1429
Cdd:PRK10953   552 VCGDANrMAKDVEQALLEVIAEFGGMDTEAADEFLSELRVERRYQRDVY 600
PRK06214 PRK06214
sulfite reductase subunit alpha;
1029-1429 2.51e-63

sulfite reductase subunit alpha;


Pssm-ID: 235745 [Multi-domain]  Cd Length: 530  Bit Score: 226.11  E-value: 2.51e-63
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1029 ARLLSRQNLQSPKSSRST--IFVRLHTNGnqeLQYQPGDHLGVFPGNHEDLVNALIERLedAPPANHVVKVEMLEE---R 1103
Cdd:PRK06214   171 ATFLSRRRLNKPGSEKETwhVEIDLAGSG---LDYEVGDSLGLFPANDPALVDAVIAAL--GAPPEFPIGGKTLREallE 245
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1104 NTALGvisnwkdesrlppctifqafkyyldittpPTPLQLQQFASLATNEKEKQRLLVLSKGlqeyeEWKWGKNPTM--V 1181
Cdd:PRK06214   246 DVSLG-----------------------------PAPDGLFELLSYITGGAARKKARALAAG-----EDPDGDAATLdvL 291
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1182 EVLEEFPSIQMPATLLLTQLSLLQPRYYSISSSPDMYPDEVHLTVAIVSYHTRdgeGPVHHGVCSSWL-NRIQADDVVPC 1260
Cdd:PRK06214   292 AALEKFPGIRPDPEAFVEALDPLQPRLYSISSSPKATPGRVSLTVDAVRYEIG---SRLRLGVASTFLgERLAPGTRVRV 368
                          250       260       270       280       290       300       310       320
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1261 FVRGAPSFHLPRNPQVPCILVGPGTGIAPFRSFWQQRQfDIQHKGMNpcpmVLVFGCRQSKIDHIYREETLQAKNKGVFR 1340
Cdd:PRK06214   369 YVQKAHGFALPADPNTPIIMVGPGTGIAPFRAFLHERA-ATKAPGRN----WLFFGHQRSATDFFYEDELNGLKAAGVLT 443
                          330       340       350       360       370       380       390       400
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1341 ELYTAYSREPDRpKKYVQDVLQEQLAEsVYRALkEQGGHIYVCGDVT-MAADVLKAIQRIMTQQGKLSEEDAGVFISRLR 1419
Cdd:PRK06214   444 RLSLAWSRDGEE-KTYVQDRMRENGAE-LWKWL-EEGAHFYVCGDAKrMAKDVERALVDIVAQFGGRSPDEAVAFVAELK 520
                          410
                   ....*....|
gi 1958667836 1420 DDNRYHEDIF 1429
Cdd:PRK06214   521 KAGRYQADVY 530
FNR_like cd00322
Ferredoxin reductase (FNR), an FAD and NAD(P) binding protein, was intially identified as a ...
1206-1409 4.08e-36

Ferredoxin reductase (FNR), an FAD and NAD(P) binding protein, was intially identified as a chloroplast reductase activity, catalyzing the electron transfer from reduced iron-sulfur protein ferredoxin to NADP+ as the final step in the electron transport mechanism of photosystem I. FNR transfers electrons from reduced ferredoxin to FAD (forming FADH2 via a semiquinone intermediate) and then transfers a hydride ion to convert NADP+ to NADPH. FNR has since been shown to utilize a variety of electron acceptors and donors and has a variety of physiological functions including nitrogen assimilation, dinitrogen fixation, steroid hydroxylation, fatty acid metabolism, oxygenase activity, and methane assimilation in many organisms. FNR has an NAD(P)-binding sub-domain of the alpha/beta class and a discrete (usually N-terminal) flavin sub-domain which vary in orientation with respect to the NAD(P) binding domain. The N-terminal moeity may contain a flavin prosthetic group (as in flavoenzymes) or use flavin as a substrate. Because flavins such as FAD can exist in oxidized, semiquinone (one- electron reduced), or fully reduced hydroquinone forms, FNR can interact with one and 2 electron carriers. FNR has a strong preference for NADP(H) vs NAD(H).


Pssm-ID: 99778 [Multi-domain]  Cd Length: 223  Bit Score: 136.81  E-value: 4.08e-36
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1206 PRYYSISSSPDMyPDEVHLTVAIVSyhtrdgegpvhHGVCSSWLNRIQADDVVPCFVRGAPSFhLPRNPQVPCILVGPGT 1285
Cdd:cd00322     41 RRAYSIASSPDE-EGELELTVKIVP-----------GGPFSAWLHDLKPGDEVEVSGPGGDFF-LPLEESGPVVLIAGGI 107
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1286 GIAPFRSFWQQRQFDIqhkgmNPCPMVLVFGCRQSKiDHIYREETLQAKNKGVFRELYTAYSREPDRPKKYVQDVLQEQL 1365
Cdd:cd00322    108 GITPFRSMLRHLAADK-----PGGEITLLYGARTPA-DLLFLDELEELAKEGPNFRLVLALSRESEAKLGPGGRIDREAE 181
                          170       180       190       200
                   ....*....|....*....|....*....|....*....|....
gi 1958667836 1366 AESvyRALKEQGGHIYVCGDVTMAADVLKAIQRIMTQQGKLSEE 1409
Cdd:cd00322    182 ILA--LLPDDSGALVYICGPPAMAKAVREALVSLGVPEERIHTE 223
SiR_like2 cd06201
Cytochrome p450- like alpha subunits of E. coli sulfite reductase (SiR) multimerize with beta ...
1206-1429 7.79e-34

Cytochrome p450- like alpha subunits of E. coli sulfite reductase (SiR) multimerize with beta subunits to catalyze the NADPH dependent reduction of sulfite to sulfide. Beta subunits have an Fe4S4 cluster and a siroheme, while the alpha subunits (cysJ gene) are of the cytochrome p450 (CyPor) family having FAD and FMN as prosthetic groups and utilizing NADPH. Cypor (including cyt -450 reductase, nitric oxide synthase, and methionine synthase reductase) are ferredoxin reductase (FNR)-like proteins with an additional N-terminal FMN domain and a connecting sub-domain inserted within the flavin binding portion of the FNR-like domain. The connecting domain orients the N-terminal FMN domain with the C-terminal FNR domain. NADPH cytochrome p450 reductase (CYPOR) serves as an electron donor in several oxygenase systems and is a component of nitric oxide synthases and methionine synthase reductases. CYPOR transfers two electrons from NADPH to the heme of cytochrome p450 via FAD and FMN. Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria in which they participate in a wide variety of redox metabolic pathways. The C-terminal domain contains most of the NADP(H) binding residues and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule which lies largely in a large gap betweed the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2 which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99798 [Multi-domain]  Cd Length: 289  Bit Score: 132.45  E-value: 7.79e-34
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1206 PRYYSISSSpdmypdevhltvaivsyhTRDG--EGPVH---HGVCSSWLNRIQADDVVPCFVRGAPSFHLPRNpQVPCIL 1280
Cdd:cd06201    100 PRFYSLASS------------------SSDGflEICVRkhpGGLCSGYLHGLKPGDTIKAFIRPNPSFRPAKG-AAPVIL 160
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1281 VGPGTGIAPFRSFwqQRQFDIQHkgmnpcPMVLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAYSREPDrpKKYVQDV 1360
Cdd:cd06201    161 IGAGTGIAPLAGF--IRANAARR------PMHLYWGGRDPASDFLYEDELDQYLADGRLTQLHTAFSRTPD--GAYVQDR 230
                          170       180       190       200       210       220
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....
gi 1958667836 1361 LQEQlAESVyRALKEQGGHIYVCGDVTMAADVLKAIQRIMTQQGklseedAGVFISRLrdDNRYHEDIF 1429
Cdd:cd06201    231 LRAD-AERL-RRLIEDGAQIMVCGSRAMAQGVAAVLEEILAPQP------LSLDELKL--QGRYAEDVY 289
SiR_like1 cd06200
Cytochrome p450- like alpha subunits of E. coli sulfite reductase (SiR) multimerize with beta ...
1206-1429 2.69e-30

Cytochrome p450- like alpha subunits of E. coli sulfite reductase (SiR) multimerize with beta subunits to catalyze the NADPH dependent reduction of sulfite to sulfide. Beta subunits have an Fe4S4 cluster and a siroheme, while the alpha subunits (cysJ gene) are of the cytochrome p450 (CyPor) family having FAD and FMN as prosthetic groups and utilizing NADPH. Cypor (including cyt -450 reductase, nitric oxide synthase, and methionine synthase reductase) are ferredoxin reductase (FNR)-like proteins with an additional N-terminal FMN domain and a connecting sub-domain inserted within the flavin binding portion of the FNR-like domain. The connecting domain orients the N-terminal FMN domain with the C-terminal FNR domain. NADPH cytochrome p450 reductase (CYPOR) serves as an electron donor in several oxygenase systems and is a component of nitric oxide synthases and methionine synthase reductases. CYPOR transfers two electrons from NADPH to the heme of cytochrome p450 via FAD and FMN. Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria in which they participate in a wide variety of redox metabolic pathways. The C-terminal domain contains most of the NADP(H) binding residues, and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule, which lies largely in a large gap betweed the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2 which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99797  Cd Length: 245  Bit Score: 120.85  E-value: 2.69e-30
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1206 PRYYSISSSPDmypD-EVHLtvaIVSYHTRDGEGPvhhGVCSSWLNRIQAD-DVVPCFVRGAPSFHLPrNPQVPCILVGP 1283
Cdd:cd06200     48 HREYSIASLPA---DgALEL---LVRQVRHADGGL---GLGSGWLTRHAPIgASVALRLRENPGFHLP-DDGRPLILIGN 117
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1284 GTGIAPFRSFWQQRQFDIQHKGMnpcpmvLVFGCRQSKIDHIYREETLQAKNKGVFRELYTAYSREPDRpKKYVQDVLQE 1363
Cdd:cd06200    118 GTGLAGLRSHLRARARAGRHRNW------LLFGERQAAHDFFCREELEAWQAAGHLARLDLAFSRDQAQ-KRYVQDRLRA 190
                          170       180       190       200       210       220
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1958667836 1364 QLAEsvYRALKEQGGHIYVCGDV-TMAADVLKAIQRIMTQQGKlseedagvfiSRLRDDNRYHEDIF 1429
Cdd:cd06200    191 AADE--LRAWVAEGAAIYVCGSLqGMAPGVDAVLDEILGEEAV----------EALLAAGRYRRDVY 245
Flavodoxin_1 pfam00258
Flavodoxin;
757-964 2.36e-29

Flavodoxin;


Pssm-ID: 425562 [Multi-domain]  Cd Length: 142  Bit Score: 114.77  E-value: 2.36e-29
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  757 ILYATETGKSQAYAKTLCEIFK-HAFDAKAMSMEEYDIV--HLEHEALVLVVTSTFGNGDPPENGEKFgCALMEMrhpns 833
Cdd:pfam00258    1 IFYGSQTGNTEKLAEAIAEGLGeAGFEVDVVDLDDVDETlsEIEEEDLLLVVVSTWGEGEPPDNAKPF-VDWLLL----- 74
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836  834 vqeerkypeplrFFPRKGPSLShvdseahslvaardsqhrsykvrfnsvssysdsrkssgdgpdlrdnfestgplaNVRF 913
Cdd:pfam00258   75 ------------FGTLEDGDLS------------------------------------------------------GLKY 88
                          170       180       190       200       210
                   ....*....|....*....|....*....|....*....|....*....|....
gi 1958667836  914 SVFGLGSRAYPHFCAFGHAVDTLLEELGGERILKMREGDEL---CGQEEAFRTW 964
Cdd:pfam00258   89 AVFGLGDSGYEGFCGAAKKLDEKLSELGASRVGPLGEGDEDpqeDGLEEAFEAW 142
CYPOR_like_FNR cd06208
These ferredoxin reductases are related to the NADPH cytochrome p450 reductases (CYPOR), but ...
1206-1425 5.48e-28

These ferredoxin reductases are related to the NADPH cytochrome p450 reductases (CYPOR), but lack the FAD-binding region connecting sub-domain. Ferredoxin-NADP+ reductase (FNR) is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins, such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria in which they participate in a wide variety of redox metabolic pathways. The C-terminal domain contains most of the NADP(H) binding residues and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule which lies largely in a large gap between the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2, which then transfers two electrons and a proton to NADP+ to form NADPH. CYPOR serves as an electron donor in several oxygenase systems and is a component of nitric oxide synthases, sulfite reducatase, and methionine synthase reductases. CYPOR transfers two electrons from NADPH to the heme of cytochrome p450 via FAD and FMN. CYPOR has a C-terminal FNR-like FAD and NAD binding module, an FMN-binding domain, and an additional connecting domain (inserted within the FAD binding region) that orients the FNR and FMN -binding domains. The C-terminal domain contains most of the NADP(H) binding residues, and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule, which lies largely in a large gap betweed the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2 which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99804 [Multi-domain]  Cd Length: 286  Bit Score: 115.50  E-value: 5.48e-28
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1206 PRYYSISSSPDM---YPDEVHLTVAIVSYhTRDGEGPVHHGVCSSWLNRIQADDVVpcFVRGaPS---FHLPRNPQVPCI 1279
Cdd:cd06208     64 LRLYSIASSRYGddgDGKTLSLCVKRLVY-TDPETDETKKGVCSNYLCDLKPGDDV--QITG-PVgktMLLPEDPNATLI 139
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1280 LVGPGTGIAPFRSFWQQRQF----DIQHKGMnpcpMVLVFGCRQSKiDHIYREE--TLQAKNKGVFReLYTAYSREPDR- 1352
Cdd:cd06208    140 MIATGTGIAPFRSFLRRLFRekhaDYKFTGL----AWLFFGVPNSD-SLLYDDEleKYPKQYPDNFR-IDYAFSREQKNa 213
                          170       180       190       200       210       220       230
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*
gi 1958667836 1353 --PKKYVQDVLQEQlAESVYRALKEQGGHIYVCGDVTMAADVLKAIQRIMtqQGKLSEEDagvFISRLRDDNRYH 1425
Cdd:cd06208    214 dgGKMYVQDRIAEY-AEEIWNLLDKDNTHVYICGLKGMEPGVDDALTSVA--EGGLAWEE---FWESLKKKGRWH 282
NAD_binding_1 pfam00175
Oxidoreductase NAD-binding domain; Xanthine dehydrogenases, that also bind FAD/NAD, have ...
1280-1394 2.46e-26

Oxidoreductase NAD-binding domain; Xanthine dehydrogenases, that also bind FAD/NAD, have essentially no similarity.


Pssm-ID: 425503 [Multi-domain]  Cd Length: 109  Bit Score: 104.65  E-value: 2.46e-26
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1280 LVGPGTGIAPFRSFWQQRQFDIQHKGmnpcPMVLVFGCRQSKiDHIYREE--TLQAKNKGVFReLYTAYSREPDRP---K 1354
Cdd:pfam00175    1 MIAGGTGIAPVRSMLRAILEDPKDPT----QVVLVFGNRNED-DILYREEldELAEKHPGRLT-VVYVVSRPEAGWtggK 74
                           90       100       110       120
                   ....*....|....*....|....*....|....*....|
gi 1958667836 1355 KYVQDVLQEQLAEsvyraLKEQGGHIYVCGDVTMAADVLK 1394
Cdd:pfam00175   75 GRVQDALLEDHLS-----LPDEETHVYVCGPPGMIKAVRK 109
PDZ_canonical cd00136
canonical PDZ domain; Canonical PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs ...
18-98 1.58e-17

canonical PDZ domain; Canonical PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain. PDZ domains usually bind to short specific peptide sequences located at the C-terminal end of their partner proteins known as PDZ binding motifs. These domains can also interact with internal peptide motifs and certain lipids, and can take part in a head-to-tail oligomerization with other PDZ domains. The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. The canonical PDZ domain contains six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467153 [Multi-domain]  Cd Length: 81  Bit Score: 78.74  E-value: 1.58e-17
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   18 VRLFKRKVGGLGF-LVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRgiASETHVVLI 96
Cdd:cd00136      2 VTLEKDPGGGLGFsIRGGKDGGGGIFVSRVEPGGPAARDGRLRVGDRILEVNGVSLEGLTHEEAVELLK--SAGGEVTLT 79

                   ..
gi 1958667836   97 LR 98
Cdd:cd00136     80 VR 81
Fpr COG1018
Flavodoxin/ferredoxin--NADP reductase [Energy production and conversion];
1207-1395 4.48e-17

Flavodoxin/ferredoxin--NADP reductase [Energy production and conversion];


Pssm-ID: 440641 [Multi-domain]  Cd Length: 231  Bit Score: 82.14  E-value: 4.48e-17
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1207 RYYSISSSPDmypdEVHLTVAIVsyhtRDGEGPVhhgvcSSWLN-RIQADDVVpcFVRGaPS--FHLPRNPQVPCILVGP 1283
Cdd:COG1018     53 RAYSLSSAPG----DGRLEITVK----RVPGGGG-----SNWLHdHLKVGDTL--EVSG-PRgdFVLDPEPARPLLLIAG 116
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1284 GTGIAPFRSFWQqrqfDIQHKGMNPcPMVLVFGCRQSKiDHIYREE--TLQAKNKGVfrELYTAYSREPDRPKKYV-QDV 1360
Cdd:COG1018    117 GIGITPFLSMLR----TLLARGPFR-PVTLVYGARSPA-DLAFRDEleALAARHPRL--RLHPVLSREPAGLQGRLdAEL 188
                          170       180       190
                   ....*....|....*....|....*....|....*
gi 1958667836 1361 LQEQLAEsvyralkEQGGHIYVCGDVTMAADVLKA 1395
Cdd:COG1018    189 LAALLPD-------PADAHVYLCGPPPMMEAVRAA 216
PDZ pfam00595
PDZ domain; PDZ domains are found in diverse signaling proteins.
17-96 1.72e-16

PDZ domain; PDZ domains are found in diverse signaling proteins.


Pssm-ID: 395476 [Multi-domain]  Cd Length: 81  Bit Score: 75.78  E-value: 1.72e-16
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   17 SVRLFKRKVGGLGFLVKERVSK--PPVIISDLIRGGAAEQSGlIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVV 94
Cdd:pfam00595    1 QVTLEKDGRGGLGFSLKGGSDQgdPGIFVSEVLPGGAAEAGG-LKVGDRILSINGQDVENMTHEEAVLALKGSGGKVTLT 79

                   ..
gi 1958667836   95 LI 96
Cdd:pfam00595   80 IL 81
PLN03116 PLN03116
ferredoxin--NADP+ reductase; Provisional
1206-1429 1.96e-15

ferredoxin--NADP+ reductase; Provisional


Pssm-ID: 215586 [Multi-domain]  Cd Length: 307  Bit Score: 78.99  E-value: 1.96e-15
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1206 PRYYSISSSpdMYPDEVHLTVA------IVSYHTRDG-EGPVHHGVCSSWLNRIQADDVVPCFVRGAPSFHLP-RNPQVP 1277
Cdd:PLN03116    81 VRLYSIAST--RYGDDFDGKTAslcvrrAVYYDPETGkEDPAKKGVCSNFLCDAKPGDKVQITGPSGKVMLLPeEDPNAT 158
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1278 CILVGPGTGIAPFRSFWqQRQF-----DIQHKGMnpcpMVLVFGCRQSKiDHIYREE--TLQAKNKGVFReLYTAYSRE- 1349
Cdd:PLN03116   159 HIMVATGTGIAPFRGFL-RRMFmedvpAFKFGGL----AWLFLGVANSD-SLLYDDEfeRYLKDYPDNFR-YDYALSREq 231
                          170       180       190       200       210       220       230       240
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1350 --PDRPKKYVQDVLqEQLAESVYRALkEQGGHIYVCGDVTMAADVLKAIQRIMTQQGKLSEEdagvFISRLRDDNRYHED 1427
Cdd:PLN03116   232 knKKGGKMYVQDKI-EEYSDEIFKLL-DNGAHIYFCGLKGMMPGIQDTLKRVAEERGESWEE----KLSGLKKNKQWHVE 305

                   ..
gi 1958667836 1428 IF 1429
Cdd:PLN03116   306 VY 307
PDZ3_PTPN13_FRMPD2-like cd06695
PDZ domain 3 of protein tyrosine phosphatase non-receptor type 13 (PTPN13), FERM and PDZ ...
18-95 1.86e-14

PDZ domain 3 of protein tyrosine phosphatase non-receptor type 13 (PTPN13), FERM and PDZ domain-containing protein 2 (FRMPD2), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 3 of PTPN13 [also known as Fas-associated protein-tyrosine phosphatase 1 (FAP-1), protein-tyrosine phosphatase 1E (PTP-E1), and protein-tyrosine phosphatase (PTPL1)], FRMPD2 (also known as PDZ domain-containing protein 4; PDZ domain-containing protein 5C), and related domains. PTPN13 regulates negative apoptotic signaling and mediates phosphoinositide 3-kinase (PI3K) signaling. PTPN13 has five PDZ domains. Proteins known to interact with PTPN13 PDZ domains include: PLEKHA1 and PLEKHA2 via PTPN13-PDZ domain 1, Fas receptor and thyroid receptor-interacting protein 6 via PTPN13-PDZ domain 2, nerve growth factor receptor and protein kinase N2 via PTPN13-PDZ domain 3, PDZ and LIM domain 4 (PDLIM4) via PTPN13-PDZ domains 2 and 4, and brain calpain-2 via PTPN13-PDZ domains 3, 4 and 5. Calpain-2-mediated PTPN13 fragments may be involved in abnormal tau aggregation and increased risk for Alzheimer's disease. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). FRMPD2 is localized in the basolateral membranes of polarized epithelial cells and is associated with tight junction formation and immune response; it contains 3 PDZ domains). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PTPN13 family PDZ3 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467181 [Multi-domain]  Cd Length: 90  Bit Score: 70.37  E-value: 1.86e-14
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   18 VRLFKRKvGGLGF-LVKERVSKPPVIISDLIR------GGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASE 90
Cdd:cd06695      4 VKLTKGS-SGLGFsFLGGENNSPEDPFSGLVRikklfpGQPAAESGLIQEGDVILAVNGEPLKGLSYQEVLSLLRGAPPE 82

                   ....*
gi 1958667836   91 THVVL 95
Cdd:cd06695     83 VTLLL 87
PDZ smart00228
Domain present in PSD-95, Dlg, and ZO-1/2; Also called DHR (Dlg homologous region) or GLGF ...
14-100 5.54e-14

Domain present in PSD-95, Dlg, and ZO-1/2; Also called DHR (Dlg homologous region) or GLGF (relatively well conserved tetrapeptide in these domains). Some PDZs have been shown to bind C-terminal polypeptides; others appear to bind internal (non-C-terminal) polypeptides. Different PDZs possess different binding specificities.


Pssm-ID: 214570 [Multi-domain]  Cd Length: 85  Bit Score: 68.56  E-value: 5.54e-14
                            10        20        30        40        50        60        70        80
                    ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836    14 NVISVRLFKRKvGGLGF-LVKERVSKPPVIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVDLSYDSALEVLRGiASETH 92
Cdd:smart00228    1 EPRLVELEKGG-GGLGFsLVGGKDEGGGVVVSSVVPGSPAAKAGL-RVGDVILEVNGTSVEGLTHLEAVDLLKK-AGGKV 77

                    ....*...
gi 1958667836    93 VVLILRGP 100
Cdd:smart00228   78 TLTVLRGG 85
FNR1 cd06195
Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible ...
1207-1398 8.04e-14

Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria in which they participate in a wide variety of redox metabolic pathways. The C-terminal domain contains most of the NADP(H) binding residues and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule which lies largely in a large gap betweed the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2 which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99792 [Multi-domain]  Cd Length: 241  Bit Score: 72.98  E-value: 8.04e-14
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1207 RYYSISSSPDmypdEVHLTVAIVsyHTRDGEgpvhhgvCSSWLNRIQADDVVpcFVRGAPSFHLPRNPQVPC---ILVGP 1283
Cdd:cd06195     45 RAYSIASAPY----EENLEFYII--LVPDGP-------LTPRLFKLKPGDTI--YVGKKPTGFLTLDEVPPGkrlWLLAT 109
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1284 GTGIAPFRSFWQQ----RQFDiqhkgmnpcPMVLVFGCRQSKiDHIYREE--TLQAKNKGVFReLYTAYSREPDRP--KK 1355
Cdd:cd06195    110 GTGIAPFLSMLRDleiwERFD---------KIVLVHGVRYAE-ELAYQDEieALAKQYNGKFR-YVPIVSREKENGalTG 178
                          170       180       190       200
                   ....*....|....*....|....*....|....*....|....
gi 1958667836 1356 YVQDVLQ-EQLAESVYRALKEQGGHIYVCGDVTMAADVLKAIQR 1398
Cdd:cd06195    179 RIPDLIEsGELEEHAGLPLDPETSHVMLCGNPQMIDDTQELLKE 222
PDZ_syntrophin-like cd06801
PDZ domain of syntrophins, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), ...
17-98 2.68e-12

PDZ domain of syntrophins, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of syntrophins (including alpha-1-syntrophin, beta-1-syntrophin, beta-2-syntrophin, gamma-1-syntrophin, and gamma-2-syntrophin), and related domains. Syntrophins play a role in recruiting various signaling molecules into signaling complexes and help provide appropriate spatiotemporal regulation of signaling pathways. They function in cytoskeletal organization and maintenance; as components of the dystrophin-glycoprotein complex (DGC), they help maintain structural integrity of skeletal muscle fibers. They link voltage-gated sodium channels to the actin cytoskeleton and the extracellular matrix, and control the localization and activity of the actin reorganizing proteins such as PI3K, PI(3,4)P2 and TAPP1. Through association with various cytoskeletal proteins within the cells, they are involved in processes such as regulation of focal adhesions, myogenesis, calcium homeostasis, and cell migration. They also have roles in synapse formation and in the organization of utrophin, acetylcholine receptor, and acetylcholinesterase at the neuromuscular synapse. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This syntrophin-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467262 [Multi-domain]  Cd Length: 83  Bit Score: 63.75  E-value: 2.68e-12
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   17 SVRLFKRKVGGLGFLVKE-RVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGiaSETHVVL 95
Cdd:cd06801      2 TVRVVKQDVGGLGISIKGgAEHKMPILISKIFKGQAADQTGQLFVGDAILSVNGENLEDATHDEAVQALKN--AGDEVTL 79

                   ...
gi 1958667836   96 ILR 98
Cdd:cd06801     80 TVK 82
Mcr1 COG0543
NAD(P)H-flavin reductase [Coenzyme transport and metabolism, Energy production and conversion]; ...
1206-1404 4.77e-12

NAD(P)H-flavin reductase [Coenzyme transport and metabolism, Energy production and conversion];


Pssm-ID: 440309 [Multi-domain]  Cd Length: 247  Bit Score: 67.58  E-value: 4.77e-12
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1206 PRYYSISSSPDMyPDEVHLTVAIVsyhtrdgegpvhhGVCSSWLNRIQADDVVpcFVRGaP---SFHLPRNPQvPCILVG 1282
Cdd:COG0543     42 RRPFSIASAPRE-DGTIELHIRVV-------------GKGTRALAELKPGDEL--DVRG-PlgnGFPLEDSGR-PVLLVA 103
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1283 PGTGIAPFRSFwqqrqfdIQHKGMNPCPMVLVFGCRqSKIDHIYREEtlqaknkgvFREL----YTAYSREPDRPKK-YV 1357
Cdd:COG0543    104 GGTGLAPLRSL-------AEALLARGRRVTLYLGAR-TPEDLYLLDE---------LEALadfrVVVTTDDGWYGRKgFV 166
                          170       180       190       200
                   ....*....|....*....|....*....|....*....|....*..
gi 1958667836 1358 QDVLQEQLAESVYRalkeqggHIYVCGDVTMaadvLKAIQRIMTQQG 1404
Cdd:COG0543    167 TDALKELLAEDSGD-------DVYACGPPPM----MKAVAELLLERG 202
PLN03115 PLN03115
ferredoxin--NADP(+) reductase; Provisional
1207-1401 1.49e-11

ferredoxin--NADP(+) reductase; Provisional


Pssm-ID: 215585 [Multi-domain]  Cd Length: 367  Bit Score: 68.10  E-value: 1.49e-11
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1207 RYYSISSS-PDMYPDE--VHLTVAIVSYHTRDGEgpVHHGVCSSWLNRIQADDVVPCFVRGAPSFHLPRNPQVPCILVGP 1283
Cdd:PLN03115   146 RLYSIASSaLGDFGDSktVSLCVKRLVYTNDQGE--IVKGVCSNFLCDLKPGAEVKITGPVGKEMLMPKDPNATIIMLAT 223
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1284 GTGIAPFRSF-WQ---QRQFDIQHKGMnpcpMVLVFGCRQSKiDHIYREE--TLQAKNKGVFRELYtAYSREPDRP---K 1354
Cdd:PLN03115   224 GTGIAPFRSFlWKmffEKHDDYKFNGL----AWLFLGVPTSS-SLLYKEEfeKMKEKAPENFRLDF-AVSREQTNAkgeK 297
                          170       180       190       200
                   ....*....|....*....|....*....|....*....|....*..
gi 1958667836 1355 KYVQDVLQEqLAESVYRALKEQGGHIYVCGDVTMAadvlKAIQRIMT 1401
Cdd:PLN03115   298 MYIQTRMAE-YAEELWELLKKDNTYVYMCGLKGME----KGIDDIMV 339
PDZ9_MUPP1-like cd10817
PDZ domain 9 of multi-PDZ-domain protein 1 (MUPP1) and related domains; PDZ (PSD-95 ...
26-85 6.16e-11

PDZ domain 9 of multi-PDZ-domain protein 1 (MUPP1) and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 9 of MUPP1. MUPP1 and PATJ serve as scaffolding proteins linking different proteins and protein complexes involved in the organization of tight junctions and epithelial polarity. MUPP1 contains an L27 (Lin-2 and Lin-7 binding) domain and 13 PDZ domains. PATJ (also known as INAD-like) contains an L27 domain and ten PDZ domains. PATJ lacks 3 PDZ domains seen in MUPP1: PDZ6, PDZ9, and PDZ13. This MuPP1-like PDZ9 domain is therefore absent from PATJ. MUPP1 and PATJ share several binding partners, including junctional adhesion molecules (JAM), zonula occludens (ZO)-3, Pals1 (protein associated with Lin-7), Par (partitioning defective)-6 proteins, and nectins (adherence junction adhesion molecules). PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MUPP1-like family PDZ9 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467263 [Multi-domain]  Cd Length: 79  Bit Score: 59.67  E-value: 6.16e-11
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   26 GGLGFLVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLR 85
Cdd:cd10817      9 GGLGIAISEEDTENGIVIKSLTEGGPAAKDGRLKVGDQILAVDDESVVGCPYEKAISLLK 68
PDZ5_GRIP1-2-like cd06682
PDZ domain 5 of glutamate receptor-interacting protein 1 (GRIP1) and GRIP2, and related ...
18-98 2.33e-10

PDZ domain 5 of glutamate receptor-interacting protein 1 (GRIP1) and GRIP2, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of alpha-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptor (AMPAR) binding proteins GRIP1 (ABP/GRIP2) and GRIP2, and related domains. GRIP1 and GRIP2 each have 7 PDZ domains. The interaction of GRIP1 and GRIP2 with GluA2/3 (AMPAR subunit) regulates AMPAR trafficking and synaptic targeting. GRIP1 has an essential role in regulating AMPAR trafficking during synaptic plasticity and learning and memory. GRIP1 and GRIP2 interact with a variety of other proteins associated with protein trafficking and internalization, for example GRIP1 also interacts with KIF5 (also known as kinesin 1), EphB receptors, scaffold protein liprin-alpha, and the rasGEF GRASP-1. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This GRIP family domain PDZ5 is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467170 [Multi-domain]  Cd Length: 85  Bit Score: 58.51  E-value: 2.33e-10
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   18 VRLFKRKVGGLGFLV---KERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRgiASETHVV 94
Cdd:cd06682      3 VKLPKRSGVGLGITIsapKNRKPGDPLIISDVKKGSVAHRTGTLEPGDKLLAIDNIRLDNCSMEDAAQILQ--QAEDIVK 80

                   ....
gi 1958667836   95 LILR 98
Cdd:cd06682     81 LKIR 84
CtpA COG0793
C-terminal processing protease CtpA/Prc, contains a PDZ domain [Posttranslational modification, ...
22-123 3.65e-10

C-terminal processing protease CtpA/Prc, contains a PDZ domain [Posttranslational modification, protein turnover, chaperones];


Pssm-ID: 440556 [Multi-domain]  Cd Length: 341  Bit Score: 63.35  E-value: 3.65e-10
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   22 KRKVGGLGFLVKERvsKPPVIISDLIRGGAAEQSGlIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVVLILRGpe 101
Cdd:COG0793     56 SGEFGGLGAELGEE--DGKVVVVSVIPGSPAEKAG-IKPGDIILAIDGKSVAGLTLDDAVKLLRGKAGTKVTLTIKRP-- 130
                           90       100
                   ....*....|....*....|..
gi 1958667836  102 gftthlettftGDGTPKTIRVT 123
Cdd:COG0793    131 -----------GEGEPITVTLT 141
O2ase_reductase_like cd06187
The oxygenase reductase FAD/NADH binding domain acts as part of the multi-component bacterial ...
1206-1395 4.80e-10

The oxygenase reductase FAD/NADH binding domain acts as part of the multi-component bacterial oxygenases which oxidize hydrocarbons using oxygen as the oxidant. Electron transfer is from NADH via FAD (in the oxygenase reductase) and an [2FE-2S] ferredoxin center (fused to the FAD/NADH domain and/or discrete) to the oxygenase. Dioxygenases add both atoms of oxygen to the substrate, while mono-oxygenases (aka mixed oxygenases) add one atom to the substrate and one atom to water. In dioxygenases, Class I enzymes are 2 component, containing a reductase with Rieske type [2Fe-2S] redox centers and an oxygenase. Class II are 3 component, having discrete flavin and ferredoxin proteins and an oxygenase. Class III have 2 [2Fe-2S] centers, one fused to the flavin domain and the other separate.


Pssm-ID: 99784 [Multi-domain]  Cd Length: 224  Bit Score: 61.45  E-value: 4.80e-10
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1206 PRYYSISSSPDmyPDevhltvAIVSYHTRDGEGpvhhGVCSSWL-NRIQADDVVpcfVRGAP--SFHLPRNPQVPCILVG 1282
Cdd:cd06187     41 WRAYSPANPPN--ED------GEIEFHVRAVPG----GRVSNALhDELKVGDRV---RLSGPygTFYLRRDHDRPVLCIA 105
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1283 PGTGIAPFRSFWQqrqfDIQHKGMNPcPMVLVFGCRQSkiDHIYREETLQ--AKNKGVFReLYTAYSREPDR---PKKYV 1357
Cdd:cd06187    106 GGTGLAPLRAIVE----DALRRGEPR-PVHLFFGARTE--RDLYDLEGLLalAARHPWLR-VVPVVSHEEGAwtgRRGLV 177
                          170       180       190
                   ....*....|....*....|....*....|....*....
gi 1958667836 1358 QDVlqeqlaesVYRALKEQGGH-IYVCGDVTMAADVLKA 1395
Cdd:cd06187    178 TDV--------VGRDGPDWADHdIYICGPPAMVDATVDA 208
cpPDZ_CPP-like cd06782
circularly permuted PDZ domain of C-terminal processing peptidase (CPP), a serine protease, ...
25-123 5.03e-10

circularly permuted PDZ domain of C-terminal processing peptidase (CPP), a serine protease, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of CPP (also known as tail-specific protease, PRC protein, Protease Re, and Photosystem II D1 protein processing peptidase), and related domains. CPP belongs to the peptidase S41A family. It cleaves a C-terminal 11 residue peptide from the precursor form of penicillin-binding protein 3, and may have a role in protecting bacterium from thermal and osmotic stresses. In the plant chloroplast, the enzyme removes the C-terminal extension of the D1 polypeptide of photosystem II. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains and as well as those with circular permutations and domain swapping of beta-strands. The canonical PDZ domain contains six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2); arranged as A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F. This CPP-like PDZ domain is a circularly permuted PDZ domain which places beta-strand A on the C-terminus. Another permutation exists in the PDZ superfamily which places both beta-strands A and B on the C-terminus.


Pssm-ID: 467623 [Multi-domain]  Cd Length: 88  Bit Score: 57.49  E-value: 5.03e-10
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   25 VGGLGFLVKERVSKPPVIISdLIRGGAAEQSGlIQAGDIILAVNDRPLVDLSYDSALEVLRGIAsETHVVL-ILRGpegf 103
Cdd:cd06782      1 FGGIGIEIGKDDDGYLVVVS-PIPGGPAEKAG-IKPGDVIVAVDGESVRGMSLDEVVKLLRGPK-GTKVKLtIRRG---- 73
                           90       100
                   ....*....|....*....|
gi 1958667836  104 tthlettftGDGTPKTIRVT 123
Cdd:cd06782     74 ---------GEGEPRDVTLT 84
PDZ4_GRIP1-2-like cd06686
PDZ domain 4 of glutamate receptor-interacting protein 1 (GRIP1) and GRIP2, and related ...
9-95 4.63e-09

PDZ domain 4 of glutamate receptor-interacting protein 1 (GRIP1) and GRIP2, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of alpha-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptor (AMPAR) binding proteins GRIP1 (ABP/GRIP2) and GRIP2, and related domains. GRIP1 and GRIP2 each have 7 PDZ domains. The interaction of GRIP1 and GRIP2 with GluA2/3 (AMPAR subunit) regulates AMPAR trafficking and synaptic targeting. GRIP1 has an essential role in regulating AMPAR trafficking during synaptic plasticity and learning and memory. GRIP1 and GRIP2 interact with a variety of other proteins associated with protein trafficking and internalization, for example GRIP1 also interacts with KIF5 (also known as kinesin 1), EphB receptors, scaffold protein liprin-alpha, and the rasGEF GRASP-1. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This GRIP family PDZ4 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467174 [Multi-domain]  Cd Length: 99  Bit Score: 55.04  E-value: 4.63e-09
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836    9 QQIQPNVISVRLFKRKVGGLGFLVK------ERVSKPPVIiSDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALE 82
Cdd:cd06686      1 QVVHTETTEVILRGDPLKGFGIQLQggvfatETLSSPPLI-SFIEPDSPAERCGVLQVGDRVLSINGIPTEDRTLEEANQ 79
                           90
                   ....*....|...
gi 1958667836   83 VLRgiASETHVVL 95
Cdd:cd06686     80 LLR--DSASKVTL 90
PDZ2-PTPN13_FRMPD2-like cd06792
PDZ domain 2 of tyrosine kinase PTPN13, FERM and PDZ domain-containing protein 2 (FRMPD2), and ...
14-95 6.07e-09

PDZ domain 2 of tyrosine kinase PTPN13, FERM and PDZ domain-containing protein 2 (FRMPD2), and similar domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 2 of human PTPN13, and related domains. PTPN13, also known as Fas-associated protein-tyrosine phosphatase 1 (FAP-1), protein-tyrosine phosphatase 1E (PTP-E1), and protein-tyrosine phosphatase (PTPL1), negatively regulates FAS-mediated apoptosis and NGFR-mediated pro-apoptotic signaling, and may also regulate phosphoinositide 3-kinase (PI3K) signaling. It contains 5 PDZ domains; interaction partners of its second PDZ domain (PDZ2) include the Fas receptor (TNFRSF6) and thyroid receptor-interacting protein 6 (TRIP6). The second PDZ (PDZ2) domain, but not PDZ1 or PDZ3, of FRMPD2 binds to GluN2A and GluN2B, two subunits of N-methyl-d-aspartic acid (NMDA) receptors. Other binding partners of the FRMPDZ2 PDZ2 domain include NOD2, and catenin family members, delta catenin (CTNND2), armadillo repeat gene deleted in velo-cardio-facial syndrome (ARVCF) and p0071 (also known as plakophilin 4; PKP4). PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PTPN13-like family PDZ2 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467254 [Multi-domain]  Cd Length: 87  Bit Score: 54.52  E-value: 6.07e-09
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   14 NVISVRLfKRKVGGLGF----LVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIAS 89
Cdd:cd06792      1 DVFEVEL-SKKDGSLGIsvtgGINTSVRHGGIYVKSLVPGGAAEQDGRIQKGDRLLEVNGVSLEGVTHKQAVECLKNAGQ 79

                   ....*.
gi 1958667836   90 ETHVVL 95
Cdd:cd06792     80 VVTLVL 85
FNR_iron_sulfur_binding_3 cd06217
Iron-sulfur binding ferredoxin reductase (FNR) proteins combine the FAD and NAD(P) binding ...
1207-1394 1.13e-08

Iron-sulfur binding ferredoxin reductase (FNR) proteins combine the FAD and NAD(P) binding regions of FNR with an iron-sulfur binding cluster domain. Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria in which they participate in a wide variety of redox metabolic pathways. The C-terminal domain contains most of the NADP(H) binding residues and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule which lies largely in a large gap between the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2 which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99813 [Multi-domain]  Cd Length: 235  Bit Score: 57.28  E-value: 1.13e-08
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1207 RYYSISSSPDMyPDEVHLTVaivsyhTRdgegpVHHGVCSSWLNRIQA-DDVVpcFVRGaP--SFHLPRNPQVPCILVGP 1283
Cdd:cd06217     51 RSYSIASSPTQ-RGRVELTV------KR-----VPGGEVSPYLHDEVKvGDLL--EVRG-PigTFTWNPLHGDPVVLLAG 115
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1284 GTGIAPFRSFWQQRqfdiQHKGMNPcPMVLVFGCRQSKiDHIYREETLQ-AKNKGVFrELYTAYSREPD----RPKKYVQ 1358
Cdd:cd06217    116 GSGIVPLMSMIRYR----RDLGWPV-PFRLLYSARTAE-DVIFRDELEQlARRHPNL-HVTEALTRAAPadwlGPAGRIT 188
                          170       180       190
                   ....*....|....*....|....*....|....*.
gi 1958667836 1359 DVLQEQLAESVyralkeQGGHIYVCGDVTMAADVLK 1394
Cdd:cd06217    189 ADLIAELVPPL------AGRRVYVCGPPAFVEAATR 218
PDZ7_PDZD2-PDZ4_hPro-IL-16-like cd06763
PDZ domain 7 of PDZ domain containing 2 (PDZD2), PDZ domain 4 of human pro-interleukin-16 ...
15-76 2.16e-08

PDZ domain 7 of PDZ domain containing 2 (PDZD2), PDZ domain 4 of human pro-interleukin-16 (isoform 1, 1332 AA), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 7 of PDZD2, also known as KIAA0300, PIN-1, PAPIN, activated in prostate cancer (AIPC) and PDZ domain-containing protein 3 (PDZK3). PDZD2 has seven PDZ domains. PDZD2 is expressed at exceptionally high levels in the pancreas and certain cancer tissues, such as prostate cancer. It promotes the proliferation of insulinoma cells and is upregulated during prostate tumorigenesis. In osteosarcoma (OS), the microRNA miR-363 acts as a tumor suppressor by inhibiting PDZD2. This family include the PDZ domain of the secreted mature form of human interleukin-16 (IL-16); this is the fourth PDZ domain (PDZ4) of human pro-interleukin-16 (isoform 1, also known as nPro-Il-16). Precursor IL-16 is cleaved to produce pro-IL-16 and C-terminal mature IL-16. Pro-IL-16 functions as a regulator of T cell growth; mature IL-16 is a CD4 ligand that induces chemotaxis and CD25 expression in CD4+ T cells. IL-16 bioactivity has been closely associated with the progression of several different cancers PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PDZD2-like family PDZ7 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467244 [Multi-domain]  Cd Length: 86  Bit Score: 53.00  E-value: 2.16e-08
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*.
gi 1958667836   15 VISVRLFKrKVGGLGFLVKERVSKP----PVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLS 76
Cdd:cd06763      1 AVTVELEK-GSAGLGFSLEGGKGSPlgdrPLTIKRIFKGGAAEQSGVLQVGDEILQINGTSLQGLT 65
PRK08105 PRK08105
flavodoxin; Provisional
893-952 2.38e-08

flavodoxin; Provisional


Pssm-ID: 181230 [Multi-domain]  Cd Length: 149  Bit Score: 54.51  E-value: 2.38e-08
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*...
gi 1958667836  893 GDGPD--------LRDNFestGPLANVRFSVFGLGSRAYPHFCAFGHAVDTLLEELGGERILKMREGD 952
Cdd:PRK08105    62 GDLPDsivplfqaLKDTA---GYQPNLRYGVIALGDSSYDNFCGAGKQFDALLQEQGAKRVGERLEID 126
PDZ1_GgSTXBP4-like cd06692
PDZ1 domain of Gallus gallus uncharacterized syntaxin-binding protein 4 (STXBP4) isoform X1, ...
41-100 3.04e-08

PDZ1 domain of Gallus gallus uncharacterized syntaxin-binding protein 4 (STXBP4) isoform X1, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of Gallus gallus uncharacterized syntaxin-binding protein 4 (STXBP4) isoform X1, and related domains. Gallus gallus STXBP4 isoform X1 contains 2 PDZ domains (PDZ1 and PDZ2). PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This STXBP4-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467179 [Multi-domain]  Cd Length: 88  Bit Score: 52.61  E-value: 3.04e-08
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|.
gi 1958667836   41 VIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHV-VLILRGP 100
Cdd:cd06692     28 IFIKRILPGGLAATDGRLKEGDLILEVNGESLQGVTNERAVSILRSASASNHMsLLIARDE 88
PDZ5_MUPP1-like cd06669
PDZ domain 5 of multi-PDZ-domain protein 1 (MUPP1), PATJ (protein-associated tight junction) ...
13-87 3.75e-08

PDZ domain 5 of multi-PDZ-domain protein 1 (MUPP1), PATJ (protein-associated tight junction) and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 5 of MUPP1 and PATJ, and related domains. MUPP1 and PATJ serve as scaffolding proteins linking different proteins and protein complexes involved in the organization of tight junctions and epithelial polarity. MUPP1 contains an L27 (Lin-2 and Lin-7 binding) domain and 13 PDZ domains. PATJ (also known as INAD-like) contains an L27 domain and ten PDZ domains. MUPP1 and PATJ share several binding partners, including junctional adhesion molecules (JAM), zonula occludens (ZO)-3, Pals1 (protein associated with Lin-7), Par (partitioning defective)-6 proteins, and nectins (adherence junction adhesion molecules). PATJ lacks 3 PDZ domains seen in MUPP1: PDZ6, 9, and 13; consequently, MUPP1 PDZ7 and 8 align with PATJ PDZ6 and 7; and MUPP1 PDZ domains 10-12 align with PATJ PDZ domains 8-10. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MUPP1-like family PDZ5 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F


Pssm-ID: 467157 [Multi-domain]  Cd Length: 98  Bit Score: 52.62  E-value: 3.75e-08
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   13 PNVISVRLFKRKvGGLGFLV-----KERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGI 87
Cdd:cd06669      6 DEVTVIELEKGD-RGLGFSIldyqdPLDPSETVIVIRSLVPGGVAEQDGRLLPGDRLVFVNDVSLENASLDEAVQALKSA 84
PDZ3_MAGI-1_3-like cd06733
PDZ domain 3 of membrane-associated guanylate kinase inverted 1 (MAGI-1), MAGI-2, and MAGI-3, ...
18-98 4.60e-08

PDZ domain 3 of membrane-associated guanylate kinase inverted 1 (MAGI-1), MAGI-2, and MAGI-3, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 3 of MAGI1, 2, 3 (MAGI is also known as Membrane-associated guanylate kinase, WW and PDZ domain-containing protein) and related domains. MAGI proteins have been implicated in the control of cell migration and invasion through altering the activity of phosphatase and tensin homolog (PTEN) and modulating Akt signaling. Four MAGI proteins have been identified (MAGI1-3 and MAGIX). MAGI1-3 have 6 PDZ domains and bind to the C-terminus of PTEN via their PDZ2 domain. MAGIX has a single PDZ domain that is related to MAGI1-3 PDZ domain 5. Other binding partners for MAGI1 include JAM4, C-terminal tail of high risk HPV-18 E6, megalin, TRAF6, Kir4.1 (basolateral K+ channel subunit), and cadherin 23; for MAGI2, include DASM1, dendrin, axin, beta- and delta-catenin, neuroligin, hyperpolarization-activated cation channels, beta1-adrenergic receptors, NMDA receptor, and TARPs; and for MAGI3 includes LPA2. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MAGI family PDZ3 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2); arranged as beta-strands A, -B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467215 [Multi-domain]  Cd Length: 85  Bit Score: 51.84  E-value: 4.60e-08
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   18 VRLfKRKVGGLGFlvkeRV-----SKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETH 92
Cdd:cd06733      4 VFL-RRQETGFGF----RIlggteEGSQVSIGAIVPGGAADLDGRLRTGDELLSVDGVNVVGASHHKVVDLMGNAARNGQ 78

                   ....*.
gi 1958667836   93 VVLILR 98
Cdd:cd06733     79 VNLTVR 84
PDZ2_PDZD7-like cd10834
PDZ domain 2 of the canonical isoform 1 of PDZ domain containing 7 (PDZD7), and related ...
41-98 6.39e-08

PDZ domain 2 of the canonical isoform 1 of PDZ domain containing 7 (PDZD7), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 2 of the long isoform 1 of PDZD7, and related domains. PDZD7 is critical for the organization of Usher syndrome type 2 (USH2) complex. Usher syndrome is the leading cause of hereditary sensory deaf-blindness in humans; USH2 is the most common sub-type. Formation of the USH2 complex is based upon heterodimerization between PDZD7 and whirlin (another PDZ domain-containing protein) and a subsequent dynamic interplay between USH2 proteins via their multiple PDZ domains. The PDZD7 PDZ2 domain binds GPR98 (also known as VLGR1) and usherin (USH2A). PDZD7 and whirlin form heterodimers through their multiple PDZ domains; whirlin and PDZD7 interact with usherin and GPR98 to form an interdependent ankle link complex. PDZD7 also interacts with myosin VIIa. PDZD7 also forms homodimers through its PDZ2 domain. Various isoforms of PDZD7 produced by alternative splicing have been identified; this subgroup includes the second PDZ domain of the canonical isoform of PDZD7- isoform 1. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PDZD7-like family PDZ2 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467270 [Multi-domain]  Cd Length: 85  Bit Score: 51.62  E-value: 6.39e-08
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*...
gi 1958667836   41 VIISDLIRGGAAEQSGlIQAGDIILAVNDRPLVDLSYDSALEVLRGiasETHVVLILR 98
Cdd:cd10834     29 IYVSKVDPGGLAEQNG-IKVGDQILAVNGVSFEDITHSKAVEVLKS---QTHLMLTIK 82
FNR_iron_sulfur_binding_2 cd06216
Iron-sulfur binding ferredoxin reductase (FNR) proteins combine the FAD and NAD(P) binding ...
1207-1392 1.07e-07

Iron-sulfur binding ferredoxin reductase (FNR) proteins combine the FAD and NAD(P) binding regions of FNR with an iron-sulfur binding cluster domain. Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria in which they participate in a wide variety of redox metabolic pathways. The C-terminal domain contains most of the NADP(H) binding residues and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule which lies largely in a large gap betweed the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2 which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99812 [Multi-domain]  Cd Length: 243  Bit Score: 54.54  E-value: 1.07e-07
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1207 RYYSISSSPDMYPDEVHLTVAIVSyhtrdgegpvhHGVCSSWL-NRIQADDVVPCfvrGAPS--FHLPRNPQVPCILVGP 1283
Cdd:cd06216     65 RSYSLSSSPTQEDGTITLTVKAQP-----------DGLVSNWLvNHLAPGDVVEL---SQPQgdFVLPDPLPPRLLLIAA 130
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1284 GTGIAPFRSFWQqrqfdiQHKGMNPCPMVLVFGCRQSKIDHIYREE--TLQAKNKGV-FRELYTAYSREpdrpkkyvQDV 1360
Cdd:cd06216    131 GSGITPVMSMLR------TLLARGPTADVVLLYYARTREDVIFADElrALAAQHPNLrLHLLYTREELD--------GRL 196
                          170       180       190
                   ....*....|....*....|....*....|..
gi 1958667836 1361 LQEQLAESVyraLKEQGGHIYVCGDVTMAADV 1392
Cdd:cd06216    197 SAAHLDAVV---PDLADRQVYACGPPGFLDAA 225
PDZ_AFDN-like cd06789
PDZ domain of afadin (AFDN), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95) ...
13-84 1.32e-07

PDZ domain of afadin (AFDN), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of afadin (AFDN, also known as ALL1-fused gene from chromosome 6 protein (AF6) and MLLT4), and related domains. AFDN belongs to the adhesion system, probably together with the E-cadherin-catenin system, that plays a role in the organization of homotypic, interneuronal, and heterotypic cell-cell adherens junctions. The AFDN PDZ domain interaction partners include poliovirus receptor-related protein PRR2/nectin, the junctional adhesion molecule (JAM), the breakpoint-cluster-region protein (BCR), connexin36 (Cx36), and a subset of Eph-related receptor tyrosine kinases; it can also bind low molecular weight ligands, in competition with a natural peptide ligand. Other AFDN-binding proteins have been identified. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This AFDN family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467251 [Multi-domain]  Cd Length: 89  Bit Score: 50.75  E-value: 1.32e-07
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*.
gi 1958667836   13 PNVISVRLFKRKvGGLGFLV----KERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVL 84
Cdd:cd06789      1 PEIITVTLKKVG-NGMGLSIvaakGAGQDKLGIYIKSVVKGGAADLDGRLQAGDQLLSVDGHSLVGLSQERAAELM 75
PDZ2_Par3-like cd23058
PDZ domain 2 of partitioning defective 3 (Par3), and related domains; PDZ (PSD-95 ...
27-97 1.87e-07

PDZ domain 2 of partitioning defective 3 (Par3), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 2 of Par3 (or PAR3 or Par-3, also known as Atypical PKC isotype-specific-interacting protein, ASIP, Drosophila Bazooka) and related domains. Par3 is a scaffold protein involved in organizing cell polarity across animals. Par3 binds numerous molecules both for its recruitment to one pole of the cell and for downstream contributions to polarized cell function. It regulates cell polarity by targeting the Par complex proteins Par6 and atypical protein kinase C (aPKC) to specific cortical sites. Physical interactions between Par3 and the Par complex include Par3 PDZ domain 1 binding to the Par6 PDZ domain, Par3 PDZ domain 1 and PDZ domain 3 binding the Par6's PDZ-binding motif, and an interaction with an undefined region of aPKC that requires both Par3 PDZ2 and PDZ3. The PDZ domains of Par3 have also been implicated as potential phosphoinositide signaling integrators, since its second PDZ domain binds to phosphoinositides, and the third PDZ interacts with phosphoinositide phosphatase PTEN. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Par3 family PDZ2 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467271 [Multi-domain]  Cd Length: 93  Bit Score: 50.33  E-value: 1.87e-07
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*
gi 1958667836   27 GLGFLVKERVS----KPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVVLIL 97
Cdd:cd23058     16 GLGFSITSRDNptggSGPIYIKNILPKGAAIQDGRLKAGDRLLEVNGVDVTGKTQEEVVSLLRSTKLGGTVSLVV 90
BenDO_FAD_NAD cd06209
Benzoate dioxygenase reductase (BenDO) FAD/NAD binding domain. Oxygenases oxidize hydrocarbons ...
1207-1388 2.00e-07

Benzoate dioxygenase reductase (BenDO) FAD/NAD binding domain. Oxygenases oxidize hydrocarbons using dioxygen as the oxidant. As a Class I bacterial dioxygenases, benzoate dioxygenase like proteins combine an [2Fe-2S] cluster containing N-terminal ferredoxin at the end fused to an FAD/NADP(P) domain. In dioxygenase FAD/NAD(P) binding domain, the reductase transfers 2 electrons from NAD(P)H to the oxygenase which insert into an aromatic substrate, an initial step in microbial aerobic degradation of aromatic rings. Flavin oxidoreductases use flavins as substrates, unlike flavoenzymes which have a flavin prosthetic group.


Pssm-ID: 99805 [Multi-domain]  Cd Length: 228  Bit Score: 53.75  E-value: 2.00e-07
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1207 RYYSISSSPDmypdEVHLTVAIvsyhtRDGEGpvhhGVCSSWL-NRIQADDVVPCfvrGAP--SFHLpRNPQVPCILVGP 1283
Cdd:cd06209     48 RSYSFSSAPG----DPRLEFLI-----RLLPG----GAMSSYLrDRAQPGDRLTL---TGPlgSFYL-REVKRPLLMLAG 110
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1284 GTGIAPFRSFWQQrqfdIQHKGMNPcPMVLVFGCRQS----KIDHIyreETLQAKNKGvFRELYTAYSREPDRPKK-YVQ 1358
Cdd:cd06209    111 GTGLAPFLSMLDV----LAEDGSAH-PVHLVYGVTRDadlvELDRL---EALAERLPG-FSFRTVVADPDSWHPRKgYVT 181
                          170       180       190
                   ....*....|....*....|....*....|
gi 1958667836 1359 DVLQEqlaesvyRALKEQGGHIYVCGDVTM 1388
Cdd:cd06209    182 DHLEA-------EDLNDGDVDVYLCGPPPM 204
PDZ2_Dlg1-2-4-like cd06724
PDZ domain 2 of human discs large homolog 1 (Dlg1), Dlg2, and Dlg4, Drosophila disc large (Dlg) ...
43-96 2.18e-07

PDZ domain 2 of human discs large homolog 1 (Dlg1), Dlg2, and Dlg4, Drosophila disc large (Dlg), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of Drosophila Dlg1, human Dlg1,2, and 4 and related domains. Dlg1 (also known as synapse-associated protein Dlg197 or SAP-97), Dlg2 (also known as channel-associated protein of synapse-110, postsynaptic density protein 93, or PSD-93), Dlg4 (also known as postsynaptic density protein 95, PSD-95, synapse-associated protein 90, or SAP-90) each have 3 PDZ domains and belong to the membrane-associated guanylate kinase family. Dlg1 regulates antigen receptor signaling and cell polarity in lymphocytes, B-cell proliferation and antibody production, and TGFalpha bioavailability; its PDZ3 domain binds pro-TGFalpha, and its PDZ2 domain binds the TACE metalloprotease responsible for cleaving pro-TGFalpha to a soluble form. Dlg2 is involved in N-methyl-D-aspartate (NMDA) receptor signaling. It regulates surface expression of NMDA receptors in dorsal horn neurons of the spinal cord, and it also interacts with NMDA receptor subunits and with Shaker-type K+ channel subunits to cluster into a channel complex. Dlg4 PDZ1 domain binds NMDA receptors, and its PDZ2 domain binds neuronal nitric oxide synthase (nNOS), forming a complex in neurons. The Drosophila Scribble complex (Scribble, Dlg, and lethal giant larvae) plays a role in apico-basal cell polarity, and in other forms of polarity, including regulation of the actin cytoskeleton, cell signaling and vesicular trafficking, and in tumor development. Postsynaptic targeting of Drosophila DLG requires interactions mediated by the first two PDZ domains. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Dlg-like family PDZ2 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467207 [Multi-domain]  Cd Length: 85  Bit Score: 49.96  E-value: 2.18e-07
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....
gi 1958667836   43 ISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVVLI 96
Cdd:cd06724     32 VTKIIEGGAAQKDGRLQVGDKLLAVNDVSLEEVTHEEAVAALKNTSDVVYLKVA 85
PDZ1_APBA1_3-like cd06720
PDZ domain 1 of amyloid-beta A4 precursor protein-binding family A member 1 (APBA1), APBA2, ...
18-95 2.34e-07

PDZ domain 1 of amyloid-beta A4 precursor protein-binding family A member 1 (APBA1), APBA2, APBA3, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of APBA1, APBA2, APBA3, and related domains. The APBA/X11/Mint protein family includes three members: neuron specific APBA1 (also known as X11alpha and Mint1) and APBA2 (also known as X11beta and Mint2), and the ubiquitously expressed APBA3 (also known as (X12gamma and Mint3). They are involved in regulating neuronal signaling, trafficking and plasticity. They contain two PDZ domains (PDZ1 and PDZ2) which bind a variety of proteins: Arf GTPases (APBA1 and APBA2 PDZ2) and neurexin (APBA1 and APBA2 PDZ1 and 2), which are involved in vesicle docking and exocytosis; alpha1B subunit of N-type Ca2+ channel (APBA1 PDZ1) that is involved in ion channels; KIF17 (APBA1 PDZ1) that is involved in transport and traffic; and Alzheimer's disease related proteins such as APP (APBA3 PDZ2), CCS (APBA1 PDZ2), NF-kappa-B/p65 (APBA2 PDZ2), presenilin-1 (APBA1 and APBA2 PDZ1 and PDZ2). PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This APBA1,2,3-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged as beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta- strand F.


Pssm-ID: 467203 [Multi-domain]  Cd Length: 86  Bit Score: 49.95  E-value: 2.34e-07
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   18 VRLFKRKVGGLGFLVKE--RVSK-PPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVV 94
Cdd:cd06720      3 VVVEKQKGEILGVVIVEsgWGSLlPTVVVANMMPGGPAARSGKLNIGDQIMSINGTSLVGLPLSTCQAIIKNLKNQTKVK 82

                   .
gi 1958667836   95 L 95
Cdd:cd06720     83 L 83
PDZ3_LNX1_2-like cd06679
PDZ domain 3 of human Ligand of Numb protein X 1 (LNX1) and LNX2, and related domains; PDZ ...
25-95 2.98e-07

PDZ domain 3 of human Ligand of Numb protein X 1 (LNX1) and LNX2, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 3 of LNX1 (also known as PDZ domain-containing RING finger protein 2, PDZRN2) and LNX2 (also known as PDZ domain-containing RING finger protein 1, PDZRN1), and related domains. LNX1 and LNX2 are Ring (Really Interesting New Gene) finger and PDZ domain-containing E3 ubiquitin ligases that bind to the cell fate determinant protein NUMB and mediate its ubiquitination. LNX1 can ubiquitinate a number of other ligands including PPFIA1, KLHL11, KIF7 and ERC2. LNX1 and LNX2 each have four PDZ domains. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This LNX family PDZ3 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467167 [Multi-domain]  Cd Length: 88  Bit Score: 49.56  E-value: 2.98e-07
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|.
gi 1958667836   25 VGGLGflvkERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVVL 95
Cdd:cd06679     18 AGGRG----SRRGDLPIYVTNVQPDGCLGRDGRIKKGDVLLSINGISLTNLSHSEAVAVLKASAASSSIVL 84
PDZ_MPP-like cd06726
PDZ domain of membrane palmitoylated proteins (MPPs), and related domains; PDZ (PSD-95 ...
28-86 6.23e-07

PDZ domain of membrane palmitoylated proteins (MPPs), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of MPP1-7 (also known as MAGUK p55 subfamily members 1-7), and related domains. MPPs comprise a subfamily of a larger group of multidomain proteins, namely, membrane-associated guanylate kinases (MAGUKs). MPPs form diverse protein complexes at the cell membranes, which are involved in a wide range of cellular processes, including establishing proper cell structure, polarity and cell adhesion. MPPs have only one PDZ domain. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MPP1-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467208 [Multi-domain]  Cd Length: 80  Bit Score: 48.42  E-value: 6.23e-07
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*....
gi 1958667836   28 LGFLVKERVSKppVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRG 86
Cdd:cd06726     13 LGATIKMEEDS--VIVARILHGGMAHRSGLLHVGDEILEINGIPVSGKTVDELQKLLSS 69
PDZ1_ZO1-like cd06727
PDZ domain 1 of Zonula Occludens-1 (ZO-1), homologs ZO-2 and ZO-3, and related domains; PDZ ...
38-85 8.97e-07

PDZ domain 1 of Zonula Occludens-1 (ZO-1), homologs ZO-2 and ZO-3, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of ZO-1, -2, -3 and related domains. Zonula occludens proteins (ZO-1, ZO-2, ZO-3) are multi-PDZ domain proteins involved in the maintenance and biogenesis of multi-protein networks at the cytoplasmic surface of intercellular contacts in epithelial and endothelial cells. They have three N-terminal PDZ domains, PDZ1-3, followed by a Src homology-3 (SH3) domain and a guanylate kinase (GuK)-like domain. Among protein-protein interactions for all ZO proteins is the binding of the first PDZ domain (PDZ1) to the C-termini of claudins, and the homo- and hetero-dimerization of ZO-proteins via their second PDZ domain (PDZ2), which takes place by symmetrical domain swapping of the first two beta-strands of PDZ2. At the cell level, ZO-1 and ZO-2 are involved in polarity maintenance, gene transcription, cell proliferation, and tumor cell metastasis. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This ZO family PDZ1 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467209 [Multi-domain]  Cd Length: 87  Bit Score: 48.42  E-value: 8.97e-07
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*...
gi 1958667836   38 KPPVIISDLIRGGAAEqsGLIQAGDIILAVNDRPLVDLSYDSALEVLR 85
Cdd:cd06727     30 DTSIVISDVLKGGPAE--GKLQENDRVVSVNGVSMENVEHSFAVQILR 75
PDZ1_Dlg1-2-4-like cd06723
PDZ domain 1 of human discs large homolog 1 (Dlg1), Dlg2, and Dlg4, Drosophila disc large (Dlg) ...
39-98 1.07e-06

PDZ domain 1 of human discs large homolog 1 (Dlg1), Dlg2, and Dlg4, Drosophila disc large (Dlg), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of Drosophila Dlg1, human Dlg1,2, and 4 and related domains. Dlg1 (also known as synapse-associated protein Dlg197 or SAP-97), Dlg2 (also known as channel-associated protein of synapse-110, postsynaptic density protein 93, or PSD-93), Dlg4 (also known as postsynaptic density protein 95, PSD-95, synapse-associated protein 90, or SAP-90) each have 3 PDZ domains and belong to the membrane-associated guanylate kinase family. Dlg1 regulates antigen receptor signaling and cell polarity in lymphocytes, B-cell proliferation and antibody production, and TGFalpha bioavailability; its PDZ3 domain binds pro-TGFalpha, and its PDZ2 domain binds the TACE metalloprotease responsible for cleaving pro-TGFalpha to a soluble form. Dlg2 is involved in N-methyl-D-aspartate (NMDA) receptor signaling. It regulates surface expression of NMDA receptors in dorsal horn neurons of the spinal cord, and it also interacts with NMDA receptor subunits and with Shaker-type K+ channel subunits to cluster into a channel complex. Dlg4 PDZ1 domain binds NMDA receptors, and its PDZ2 domain binds neuronal nitric oxide synthase (nNOS), forming a complex in neurons. The Drosophila Scribble complex (Scribble, Dlg, and lethal giant larvae) plays a role in apico-basal cell polarity, and in other forms of polarity, including regulation of the actin cytoskeleton, cell signaling and vesicular trafficking, and in tumor development. Postsynaptic targeting of Drosophila DLG requires interactions mediated by the first two PDZ domains. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Dlg-like family PDZ1 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467206 [Multi-domain]  Cd Length: 89  Bit Score: 48.08  E-value: 1.07e-06
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   39 PPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASEthVVLILR 98
Cdd:cd06723     30 PSIYITKIIPGGAAAADGRLRVNDIILRVNDVDVRNVTHSVAVEALKEAGSI--VRLYVK 87
NADH_quinone_reductase cd06188
Na+-translocating NADH:quinone oxidoreductase (Na+-NQR) FAD/NADH binding domain. (Na+-NQR) ...
1207-1396 1.19e-06

Na+-translocating NADH:quinone oxidoreductase (Na+-NQR) FAD/NADH binding domain. (Na+-NQR) provides a means of storing redox reaction energy via the transmembrane translocation of Na2+ ions. The C-terminal domain resembles ferredoxin:NADP+ oxidoreductase, and has NADH and FAD binding sites. (Na+-NQR) is distinct from H+-translocating NADH:quinone oxidoreductases and noncoupled NADH:quinone oxidoreductases. The NAD(P) binding domain of ferredoxin reductase-like proteins catalyze electron transfer between an NAD(P)-binding domain of the alpha/beta class and a discrete (usually N-terminal) domain which vary in orientation with respect to the NAD(P) binding domain. The N-terminal domain of this group typically contains an iron-sulfur cluster binding domain.


Pssm-ID: 99785 [Multi-domain]  Cd Length: 283  Bit Score: 51.92  E-value: 1.19e-06
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1207 RYYSISSSPDMyPDEVHLTVAIVSyhTRDGEGPVHHGVCSSWLNRIQADDVVPcfVRGAPSFHLPRNPQVPCILVGPGTG 1286
Cdd:cd06188     87 RAYSLANYPAE-EGELKLNVRIAT--PPPGNSDIPPGIGSSYIFNLKPGDKVT--ASGPFGEFFIKDTDREMVFIGGGAG 161
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1287 IAPFRSFWQQrqfdiQHKGMNPC-PMVLVFGCRqSKIDHIYREEtlqaknkgvFRELYTAYSR--------EPDR----- 1352
Cdd:cd06188    162 MAPLRSHIFH-----LLKTLKSKrKISFWYGAR-SLKELFYQEE---------FEALEKEFPNfkyhpvlsEPQPednwd 226
                          170       180       190       200
                   ....*....|....*....|....*....|....*....|....*
gi 1958667836 1353 -PKKYVQDVLQEQLAEsvyRALKEQGGHIYVCGDVTMAADVLKAI 1396
Cdd:cd06188    227 gYTGFIHQVLLENYLK---KHPAPEDIEFYLCGPPPMNSAVIKML 268
PDZ_Dishevelled-like cd06717
PDZ domain of segment polarity protein dishevelled homolog DVL1, DVL2, DVL3, and related ...
43-89 1.47e-06

PDZ domain of segment polarity protein dishevelled homolog DVL1, DVL2, DVL3, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of DVL1-3, and related domains. The dishevelleds (DVL1, 2 and 3 in humans) act downstream of Frizzled (FZD) receptors in both the canonical and non-canonical WNT signaling pathway; they bind the cytoplasmic C-terminus of frizzled family members and transduce the Wnt signal to down-stream effectors. They bind to several proteins known to modulate Wnt signaling. Binding partners of the DVL1 PDZ domain include nucleoredoxin (NXN), Van Gogh-like (VANGL1), Wnt receptor RYK, Dapper 1 (DACT1), Frizzled7 (FZD7), transmembrane protein 88 (TMEM88), Daple (dishevelled-associating protein with a high frequency of leucines), also known as Ccdc88c), and cysteine-rich protein Idax. The DVL2 PDZ domain has been shown to bind the nuclear export signal sequence of the DVL2 protein. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This DVL-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467201 [Multi-domain]  Cd Length: 87  Bit Score: 47.74  E-value: 1.47e-06
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*..
gi 1958667836   43 ISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIAS 89
Cdd:cd06717     30 VGSIMKGGAVAADGRIEPGDMILQVNDISFENMSNDDAVRVLREAVH 76
PDZ11_MUPP1-PDZ9_PATJ-like cd06674
PDZ domain 11 of MUPP1 of multi-PDZ-domain protein 1 (MUPP1), domain 9 of PATJ ...
14-68 1.54e-06

PDZ domain 11 of MUPP1 of multi-PDZ-domain protein 1 (MUPP1), domain 9 of PATJ (protein-associated tight junction) and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 11 of MUPP1, PDZ domain 9 of PATJ, and related domains. MUPP1 and PATJ serve as scaffolding proteins linking different proteins and protein complexes involved in the organization of tight junctions and epithelial polarity. MUPP1 contains an L27 (Lin-2 and Lin-7 binding) domain and 13 PDZ domains. PATJ (also known as INAD-like) contains an L27 domain and ten PDZ domains. MUPP1 and PATJ share several binding partners, including junctional adhesion molecules (JAM), zonula occludens (ZO)-3, Pals1 (protein associated with Lin-7), Par (partitioning defective)-6 proteins, and nectins (adherence junction adhesion molecules). PATJ lacks 3 PDZ domains seen in MUPP1: PDZ6, 9, and 13; consequently, MUPP1 PDZ7 and 8 align with PATJ PDZ6 and 7; and MUPP1 PDZ domains 10-12 align with PATJ PDZ domains 8-10. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MUPP1-like family PDZ11 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467162 [Multi-domain]  Cd Length: 87  Bit Score: 47.66  E-value: 1.54e-06
                           10        20        30        40        50
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gi 1958667836   14 NVISVRLFKRKVGGLGFLVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVN 68
Cdd:cd06674      2 DIFTVELQKKPGRGLGLSIVGKRNDTGVFVSDIVKGGAADADGRLMQGDQILSVN 56
PDZ_6 pfam17820
PDZ domain; This entry represents the PDZ domain from a wide variety of proteins.
42-98 1.59e-06

PDZ domain; This entry represents the PDZ domain from a wide variety of proteins.


Pssm-ID: 436067 [Multi-domain]  Cd Length: 54  Bit Score: 46.37  E-value: 1.59e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*..
gi 1958667836   42 IISDLIRGGAAEQSGLiQAGDIILAVNDRPLvdLSYDSALEVLRGIASETHVVLILR 98
Cdd:pfam17820    1 VVTAVVPGSPAERAGL-RVGDVILAVNGKPV--RSLEDVARLLQGSAGESVTLTVRR 54
PDZ3_MUPP1-like cd06791
PDZ domain 3 of multi-PDZ-domain protein 1 (MUPP1) and PATJ (protein-associated tight junction) ...
14-85 2.27e-06

PDZ domain 3 of multi-PDZ-domain protein 1 (MUPP1) and PATJ (protein-associated tight junction) and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 3 of MUPP1 and PATJ, and related domains. MUPP1 and PATJ serve as scaffolding proteins linking different proteins and protein complexes involved in the organization of tight junctions and epithelial polarity. MUPP1 contains an L27 (Lin-2 and Lin-7 binding) domain and 13 PDZ domains. PATJ (also known as INAD-like) contains an L27 domain and ten PDZ domains. MUPP1 and PATJ share several binding partners, including junctional adhesion molecules (JAM), zonula occludens (ZO)-3, Pals1 (protein associated with Lin-7), Par (partitioning defective)-6 proteins, and nectins (adherence junction adhesion molecules). PATJ lacks 3 PDZ domains seen in MUPP1: PDZ6, 9, and 13; consequently, MUPP1 PDZ7 and 8 align with PATJ PDZ6 and 7; and MUPP1 PDZ domains 10-12 align with PATJ PDZ domains 8-10. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MUPP1-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467253 [Multi-domain]  Cd Length: 89  Bit Score: 47.23  E-value: 2.27e-06
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gi 1958667836   14 NVISVRLFKRKVG-GL---GFLVKERVSKPPVI-ISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLR 85
Cdd:cd06791      1 ETFEVELVKDEQGlGItiaGYVGEKASGELSGIfVKSIIPGSAADQDGRIQVNDQIIAVDGVNLQGFTNQEAVEVLR 77
PDZ2_PDZD2-like cd06758
PDZ domain 2 of PDZ domain containing 2 (PDZD2), and related domains; PDZ (PSD-95 ...
41-95 2.29e-06

PDZ domain 2 of PDZ domain containing 2 (PDZD2), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 2 of PDZD2, also known as KIAA0300, PIN-1, activated in prostate cancer (AIPC) and PDZ domain-containing protein 3 (PDZK3). PDZD2 has seven PDZ domains, and is expressed at exceptionally high levels in the pancreas and certain cancer tissues such as prostate cancer. It promotes the proliferation of insulinoma cells and is upregulated during prostate tumorigenesis. In osteosarcoma (OS), the microRNA miR-363 acts as a tumor suppressor by inhibiting PDZD2. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PDZD2-like family PDZ2 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467239 [Multi-domain]  Cd Length: 88  Bit Score: 46.96  E-value: 2.29e-06
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*
gi 1958667836   41 VIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVVL 95
Cdd:cd06758     31 IFVAGVEEGGSADRDGRLKKGDELLMINGQSLIGLSHQEAVAILRSSASPVQLVI 85
PDZ3_harmonin cd06739
PDZ domain 3 of harmonin isoforms a and b, and related domains; PDZ (PSD-95 (Postsynaptic ...
18-84 2.86e-06

PDZ domain 3 of harmonin isoforms a and b, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 3 of harmonin isoforms a and b, and related domains. Harmonin (also known as Usher Type 1C, PDZ-73 and AIE-75) is a key organizer of the Usher (USH) protein interactome. USH syndrome is the leading cause of hereditary sensory deaf-blindness in humans; three clinically distinct types of USH have been identified, type 1 to 3. The gene encoding harmonin (USH1C) is the causative gene for the USH type 1C phenotype. There are at least 10 alternatively spliced isoforms of harmonin, which are divided into three subclasses (a, b, and c). All isoforms contain the first two PDZ domains and the first coiled-coil domain. The a and b isoforms all have a third PDZ domain. The different PDZ domains are responsible for interactions with all known Usher syndrome type 1 proteins, and most Usher syndrome type 2 proteins. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This harmonin family PDZ3 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467221 [Multi-domain]  Cd Length: 94  Bit Score: 46.92  E-value: 2.86e-06
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gi 1958667836   18 VRLFK-RKVGGLGFLVKERVSKP---PVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVL 84
Cdd:cd06739      3 VRLLRiKKNGPLDLALEGGIDSPlggKIVVSAVYEGGAADKHGGIVKGDQIMMVNGKSLTDVTLAEAEAAL 73
PDZ5_DrPTPN13-like cd23060
PDZ domain 5 of Danio rerio tyrosine-protein phosphatase non-receptor type 13 (Ptpn13) and ...
18-85 2.90e-06

PDZ domain 5 of Danio rerio tyrosine-protein phosphatase non-receptor type 13 (Ptpn13) and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 5 of Danio rerio Ptpn13, and related domains. Protein-tyrosine phosphatases (PTPs) dephosphorylate phosphotyrosyl residues in proteins that are phosphorylated by protein tyrosine kinases (PTKs). Danio rerio Ptpn13 is a classical non-receptor-like PTP. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PTPN13-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467273 [Multi-domain]  Cd Length: 80  Bit Score: 46.57  E-value: 2.90e-06
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                   ....*....|....*....|....*....|....*....|....*....|....*....|....*...
gi 1958667836   18 VRLFKRKVGGLGFLVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLR 85
Cdd:cd23060      2 IELEKPANGGLGFSLVGGEGGSGIFVKSISPGGVADRDGRLQVGDRLLQVNGESVIGLSHSKAVNILR 69
PDZ13_MUPP1-like cd06676
PDZ domain 13 of multi-PDZ-domain protein 1 (MUPP1) and related domains; PDZ (PSD-95 ...
22-95 3.80e-06

PDZ domain 13 of multi-PDZ-domain protein 1 (MUPP1) and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 13 of MUPP1. MUPP1 and PATJ serve as scaffolding proteins linking different proteins and protein complexes involved in the organization of tight junctions and epithelial polarity. MUPP1 contains an L27 (Lin-2 and Lin-7 binding) domain and 13 PDZ domains. PATJ (also known as INAD-like) contains an L27 domain and ten PDZ domains. PATJ lacks 3 PDZ domains seen in MUPP1: PDZ6, PDZ9, and PDZ13. This MuPP1-like PDZ13 domain is therefore absent from PATJ. MUPP1 and PATJ share several binding partners, including junctional adhesion molecules (JAM), zonula occludens (ZO)-3, Pals1 (protein associated with Lin-7), Par (partitioning defective)-6 proteins, and nectins (adherence junction adhesion molecules). PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MUPP1-like family PDZ13 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467164 [Multi-domain]  Cd Length: 83  Bit Score: 46.18  E-value: 3.80e-06
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                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*...
gi 1958667836   22 KRKVGGLGFLVKERVSKP----PVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGiaSETHVVL 95
Cdd:cd06676      5 ERGSDGLGFSIVGGFGSPhgdlPIYVKTVFEKGAAAEDGRLKRGDQILAVNGESLEGVTHEEAVNILKK--TKGTVTL 80
PDZ3_Par3-like cd23059
PDZ domain 3 of partitioning defective 3 (Par3), and related domains; PDZ (PSD-95 ...
26-91 4.84e-06

PDZ domain 3 of partitioning defective 3 (Par3), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 3 of Par3 (or PAR3 or Par-3, also known as Atypical PKC isotype-specific-interacting protein, ASIP, Drosophila Bazooka) and related domains. Par3 is a scaffold protein involved in organizing cell polarity across animals. Par3 binds numerous molecules both for its recruitment to one pole of the cell and for downstream contributions to polarized cell function. It regulates cell polarity by targeting the Par complex proteins Par6 and atypical protein kinase C (aPKC) to specific cortical sites. Physical interactions between Par-3 and the Par complex include Par3 PDZ domain 1 binding to the Par6 PDZ domain, Par3 PDZ domain 1 and PDZ domain 3 binding the Par6's PDZ-binding motif, and an interaction with an undefined region of aPKC that requires both Par3 PDZ2 and PDZ3. The PDZ domains of Par3 have also been implicated as potential phosphoinositide signaling integrators, since its second PDZ domain binds to phosphoinositides, and the third PDZ interacts with phosphoinositide phosphatase PTEN. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Par3 family PDZ3 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467272 [Multi-domain]  Cd Length: 103  Bit Score: 46.51  E-value: 4.84e-06
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gi 1958667836   26 GGLGFLVKERVSKPP--------VIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASET 91
Cdd:cd23059     16 AGLGVSVKGKTSKEDnggkadlgIFIKSIIHGGAASKDGRLRVNDQLIAVNGESLLGLTNSEAMETLRRAMSTE 89
PDZ_Par6-like cd06718
PDZ domain of partitioning defective 6 (Par6), Drosophila Rho GTPase-activating protein 100F ...
18-79 6.24e-06

PDZ domain of partitioning defective 6 (Par6), Drosophila Rho GTPase-activating protein 100F (RhoGAP100F), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of Par6 (also known as PAR6 or Par-6), RhoGAP100F, and related domains. Par6 is part of a conserved machinery that directs metazoan cell polarity, a process necessary for the function of diverse cell types. Par6 forms a cell polarity-regulatory complex with atypical protein kinase C (aPKC) and Par3. Par6 can also directly associate with PALS1 (proteins associated with Lin7, also known as Stardust) providing a link between the Par3/aPKC/Par6 complex and the PALS1-PATJ (protein-associated TJ) complex. Binding partners of the Par6-PDZ domain include Par3, PALS1/Stardust; leucine-rich repeat-containing protein netrin-G ligand-2 (NGL-2), human crumbs (CRB3) involve in the morphogenesis of the tight junctions in mammalian epithelial cells, and PAR-6 co-operates with the Par6 semi-CRIB domain to bind CDC42. CDC42 regulates the Par6 PDZ domain through an allosteric CRIB-PDZ transition. Drosophila RhoGAP100F, also known as synapse defective protein 1 homolog (syd-1 homolog), is a GTPase activator for the Rho-type GTPases by converting them to an inactive GDP-bound form. The RhoGAP100F-PDZ domain binds the neurexin C terminus to control synapse formation at the Drosophila neuromuscular junction. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Par6-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467202 [Multi-domain]  Cd Length: 84  Bit Score: 45.64  E-value: 6.24e-06
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gi 1958667836   18 VRLFKRKVGGLGFLVKERVSK---PPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDS 79
Cdd:cd06718      3 VELIKPPGKPLGFYIRDGNGVervPGIFISRLVLGSLADSTGLLAVGDEILEVNGVEVTGKSLDD 67
flavohem_like_fad_nad_binding cd06184
FAD_NAD(P)H binding domain of flavohemoglobin. Flavohemoglobins have a globin domain ...
1206-1430 6.41e-06

FAD_NAD(P)H binding domain of flavohemoglobin. Flavohemoglobins have a globin domain containing a B-type heme fused with a ferredoxin reductase-like FAD/NAD-binding domain. Flavohemoglobins detoxify nitric oxide (NO) via an NO dioxygenase reaction. The hemoglobin domain adopts a globin fold with an embedded heme molecule. Flavohemoglobins also have a C-terminal reductase domain with bindiing sites for FAD and NAD(P)H. This domain catalyzes the conversion of NO + O2 + NAD(P)H to NO3- + NAD(P)+. Instead of the oxygen transport function of hemoglobins, flavohemoglobins seem to act in NO dioxygenation and NO signalling.


Pssm-ID: 99781  Cd Length: 247  Bit Score: 49.48  E-value: 6.41e-06
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gi 1958667836 1206 PRYYSISSspdmYPDEVHLTVAIvsyhTRDGEGPVhhgvcSSWL-NRIQADDVVPCfvrGAPS--FHLPRNPQVPCILVG 1282
Cdd:cd06184     57 IRQYSLSD----APNGDYYRISV----KREPGGLV-----SNYLhDNVKVGDVLEV---SAPAgdFVLDEASDRPLVLIS 120
                           90       100       110       120       130       140       150       160
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gi 1958667836 1283 PGTGIAPFRSFwqqrqfdIQH--KGMNPCPMVLVFGCRQSKiDHIYREET--LQAKNKGVfrELYTAYSREPDRPKKyVQ 1358
Cdd:cd06184    121 AGVGITPMLSM-------LEAlaAEGPGRPVTFIHAARNSA-VHAFRDELeeLAARLPNL--KLHVFYSEPEAGDRE-ED 189
                          170       180       190       200       210       220       230
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gi 1958667836 1359 DVLQEQL-AESVYRALKEQGGHIYVCGDVTMAADVLKAIQrimtqqgklseeDAGVfisrlrDDNRYHEDIFG 1430
Cdd:cd06184    190 YDHAGRIdLALLRELLLPADADFYLCGPVPFMQAVREGLK------------ALGV------PAERIHYEVFG 244
PDZ6_GRIP1-2-like cd06683
PDZ domain 6 of glutamate receptor-interacting protein 1 (GRIP1) and GRIP2, and related ...
15-98 7.98e-06

PDZ domain 6 of glutamate receptor-interacting protein 1 (GRIP1) and GRIP2, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of alpha-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptor (AMPAR) binding proteins GRIP1 (ABP/GRIP2) and GRIP2, and related domains. GRIP1 and GRIP2 each have 7 PDZ domains. The interaction of GRIP1 and GRIP2 with GluA2/3 (AMPAR subunit) regulates AMPAR trafficking and synaptic targeting. GRIP1 has an essential role in regulating AMPAR trafficking during synaptic plasticity and learning and memory. GRIP1 and GRIP2 interact with a variety of other proteins associated with protein trafficking and internalization, for example GRIP1 also interacts with KIF5 (also known as kinesin 1), EphB receptors, scaffold protein liprin-alpha, and the rasGEF GRASP-1. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This GRIP family PDZ6 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467171 [Multi-domain]  Cd Length: 85  Bit Score: 45.37  E-value: 7.98e-06
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gi 1958667836   15 VISVRLfKRKVGGLGFLVK--ERVSKPpVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGiASETH 92
Cdd:cd06683      3 IYTVEL-KRYGGPLGITISgtEEPFDP-IVISGLTEGGLAERTGAIHVGDRILAINGESLRGKPLSEAIHLLQN-AGDTV 79

                   ....*.
gi 1958667836   93 VVLILR 98
Cdd:cd06683     80 TLKISR 85
PDZ5_MAGI-1_3-like cd06735
PDZ domain 5 of membrane-associated guanylate kinase inverted 1 (MAGI-1), MAGI-2, and MAGI-3, ...
16-98 8.72e-06

PDZ domain 5 of membrane-associated guanylate kinase inverted 1 (MAGI-1), MAGI-2, and MAGI-3, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 5 of MAGI1, 2, 3 (MAGI is also known as Membrane-associated guanylate kinase, WW and PDZ domain-containing protein) and related domains. MAGI proteins have been implicated in the control of cell migration and invasion through altering the activity of phosphatase and tensin homolog (PTEN) and modulating Akt signaling. Four MAGI proteins have been identified (MAGI1-3 and MAGIX). MAGI1-3 have 6 PDZ domains and bind to the C-terminus of PTEN via their PDZ2 domain. MAGIX has a single PDZ domain that is related to MAGI1-3 PDZ domain 5, and belongs to this MAGI1,2,3-like family. Other binding partners for MAGI1 include JAM4, C-terminal tail of high risk HPV-18 E6, megalin, TRAF6, Kir4.1 (basolateral K+ channel subunit), and cadherin 23; for MAGI2, include DASM1, dendrin, axin, beta- and delta-catenin, neuroligin, hyperpolarization-activated cation channels, beta1-adrenergic receptors, NMDA receptor, and TARPs; and for MAGI3 includes LPA2. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MAGI family PDZ5 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged as beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467217 [Multi-domain]  Cd Length: 84  Bit Score: 45.26  E-value: 8.72e-06
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gi 1958667836   16 ISVRLfKRKVGGLGFLVK--ERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRgiASETHV 93
Cdd:cd06735      2 YSVEL-ERGPKGFGFSIRggREYNNMPLYVLRLAEDGPAQRDGRLRVGDQILEINGESTQGMTHAQAIELIR--SGGSVV 78

                   ....*
gi 1958667836   94 VLILR 98
Cdd:cd06735     79 RLLLR 83
phenol_2-monooxygenase_like cd06211
Phenol 2-monooxygenase (phenol hydroxylase) is a flavoprotein monooxygenase, able to use ...
1206-1410 1.36e-05

Phenol 2-monooxygenase (phenol hydroxylase) is a flavoprotein monooxygenase, able to use molecular oxygen as a substrate in the microbial degredation of phenol. This protein is encoded by a single gene and uses a tightly bound FAD cofactor in the NAD(P)H dependent conversion of phenol and O2 to catechol and H2O. This group is related to the NAD binding ferredoxin reductases.


Pssm-ID: 99807  Cd Length: 238  Bit Score: 48.09  E-value: 1.36e-05
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1206 PRYYSISSSPDMyPDEVHLTVAIVsyhtrdgEGpvhhGVCSSWLNR-IQADDVVpcfVRGAP--SFHLPRNPQVPCILVG 1282
Cdd:cd06211     52 TRAFSIASSPSD-AGEIELHIRLV-------PG----GIATTYVHKqLKEGDEL---EISGPygDFFVRDSDQRPIIFIA 116
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1283 PGTGIAPFRSFWqqrqFDIQHKGMnPCPMVLVFGCRqSKIDHIYREETLQ-AKNKGVFRELyTAYSREPDRP-----KKY 1356
Cdd:cd06211    117 GGSGLSSPRSMI----LDLLERGD-TRKITLFFGAR-TRAELYYLDEFEAlEKDHPNFKYV-PALSREPPESnwkgfTGF 189
                          170       180       190       200       210
                   ....*....|....*....|....*....|....*....|....*....|....*.
gi 1958667836 1357 VQDVLQeqlaesvyRALKEQG-GH-IYVCGDVTMaadVLKAIQRIMtqQGKLSEED 1410
Cdd:cd06211    190 VHDAAK--------KHFKNDFrGHkAYLCGPPPM---IDACIKTLM--QGRLFERD 232
PDZ1_MUPP1-like cd06689
PDZ domain 1 of multi-PDZ-domain protein 1 (MUPP1) and PATJ (protein-associated tight junction) ...
15-95 1.44e-05

PDZ domain 1 of multi-PDZ-domain protein 1 (MUPP1) and PATJ (protein-associated tight junction), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of MUPP1 and PATJ, and related domains. MUPP1 and PATJ serve as scaffolding proteins linking different proteins and protein complexes involved in the organization of tight junctions and epithelial polarity. MUPP1 contains an L27 (Lin-2 and Lin-7 binding) domain and 13 PDZ domains. PATJ (also known as INAD-like) contains an L27 domain and ten PDZ domains. MUPP1 and PATJ share several binding partners, including junctional adhesion molecules (JAM), zonula occludens (ZO)-3, Pals1 (protein associated with Lin-7), Par (partitioning defective)-6 proteins, and nectins (adherence junction adhesion molecules). PATJ lacks 3 PDZ domains seen in MUPP1: PDZ6, 9, and 13; consequently, MUPP1 PDZ7 and 8 align with PATJ PDZ6 and 7; and MUPP1 PDZ domains 10-12 align with PATJ PDZ domains 8-10. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MUPP1-like family PDZ1 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467176 [Multi-domain]  Cd Length: 102  Bit Score: 45.31  E-value: 1.44e-05
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   15 VISVRLFKRKVGGLGFLV----KERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPL-VDLSYDSALEVLRGIAS 89
Cdd:cd06689     15 VEYIELEKPESGGLGFSVvglkSENRGELGIFVQEIQPGSVAARDGRLKENDQILAINGQPLdQSISHQQAIAILQQAKG 94

                   ....*.
gi 1958667836   90 ETHVVL 95
Cdd:cd06689     95 SVELVV 100
PDZ6_PDZD2-PDZ3_hPro-IL-16-like cd06762
PDZ domain 6 of PDZ domain containing 2 (PDZD2), PDZ domain 3 of human pro-interleukin-16 ...
18-98 1.69e-05

PDZ domain 6 of PDZ domain containing 2 (PDZD2), PDZ domain 3 of human pro-interleukin-16 (isoform 1, 1332 AA), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 6 of PDZD2, also known as KIAA0300, PIN-1, activated in prostate cancer (AIPC) and PDZ domain-containing protein 3 (PDZK3). PDZD2 has seven PDZ domains. PDZD2 is expressed at exceptionally high levels in the pancreas and certain cancer tissues, such as prostate cancer. It promotes the proliferation of insulinoma cells and is upregulated during prostate tumorigenesis. In osteosarcoma (OS), the microRNA miR-363 acts as a tumor suppressor by inhibiting PDZD2. This family also includes the third PDZ domain (PDZ3) of human pro-interleukin-16 (isoform 1, also known as nPro-IL-16). Precursor IL-16 is cleaved to produce pro-IL-16 and C-terminal mature IL-16. Pro-IL-16 functions as a regulator of T cell growth; mature IL-16 is a CD4 ligand that induces chemotaxis and CD25 expression in CD4+ T cells. IL-16 bioactivity has been closely associated with the progression of several different cancers. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PDZD2-like family PDZ6 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467243 [Multi-domain]  Cd Length: 86  Bit Score: 44.56  E-value: 1.69e-05
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   18 VRLFKRKVGGLGFLVK--ERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVVL 95
Cdd:cd06762      4 VVLHKEEGSGLGFSLAggSDLENKSITVHRVFPSGLAAQEGTIQKGDRILSINGKSLKGVTHGDALSVLKQARLPKVAVV 83

                   ...
gi 1958667836   96 ILR 98
Cdd:cd06762     84 VIR 86
FNR_iron_sulfur_binding cd06191
Iron-sulfur binding Ferredoxin Reductase (FNR) proteins combine the FAD and NAD(P) binding ...
1207-1429 1.99e-05

Iron-sulfur binding Ferredoxin Reductase (FNR) proteins combine the FAD and NAD(P) binding regions of FNR with a C-terminal iron-sulfur binding cluster domain. FNR was intially identified as a chloroplast reductase activity catalyzing the electron transfer from reduced iron-sulfur protein ferredoxin to NADP+ as the final step in the electron transport mechanism of photosystem I. FNR transfers electrons from reduced ferredoxin to FAD (forming FADH2 via a semiquinone intermediate) and then transfers a hydride ion to convert NADP+ to NADPH. FNR has since been shown to utilize a variety of electron acceptors and donors and has a variety of physiological functions including nitrogen assimilation, dinitrogen fixation, steroid hydroxylation, fatty acid metabolism, oxygenase activity, and methnae assimilation in a variety of organisms. FNR has an NAD(P)-binding sub-domain of the alpha/beta class and a discrete (usually N-terminal) flavin sub-domain which vary in orientation with respect to the NAD(P) binding domain. The N-terminal moeity may contain a flavin prosthetic group (as in flavoenzymes) or use flavin as a substrate. Because flavins such as FAD can exist in oxidized, semiquinone (one- electron reduced), or fully reduced hydroquinone forms, FNR can interact with one and 2 electron carriers. FNR has a strong preference for NADP(H) vs NAD(H).


Pssm-ID: 99788 [Multi-domain]  Cd Length: 231  Bit Score: 47.52  E-value: 1.99e-05
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1207 RYYSISSSPdmYPDEVHLTVAIVsyhtrdgEGpvhhGVCSSWLNR-IQADDVVPcfVRGAPS-FHLPRNPQVPCILVGPG 1284
Cdd:cd06191     47 RCYSLCSSP--APDEISITVKRV-------PG----GRVSNYLREhIQPGMTVE--VMGPQGhFVYQPQPPGRYLLVAAG 111
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1285 TGIAPFRSFWQQRqfdiqHKGMNPCPMVLVFGCRQSKiDHIYREETLQAKNKGVFRELYTAYSRE-PDRPKKYVQDVLQE 1363
Cdd:cd06191    112 SGITPLMAMIRAT-----LQTAPESDFTLIHSARTPA-DMIFAQELRELADKPQRLRLLCIFTREtLDSDLLHGRIDGEQ 185
                          170       180       190       200       210       220
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*.
gi 1958667836 1364 QLAESVYRALKEQggHIYVCGdvtmAADVLKAIQRIMTQQGklseedagvfisrlRDDNRYHEDIF 1429
Cdd:cd06191    186 SLGAALIPDRLER--EAFICG----PAGMMDAVETALKELG--------------MPPERIHTERF 231
PDZ_NHERF-like cd06768
PDZ domains of the Na+/H+ exchange regulatory cofactor (NHERF) family (NHERF1-4), and related ...
18-97 2.26e-05

PDZ domains of the Na+/H+ exchange regulatory cofactor (NHERF) family (NHERF1-4), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of the Na+/H+ exchange regulatory cofactor (NHERF) family of multi-PDZ-domain-containing scaffolding proteins (NHERF1-4), and related domains. The NHERF family includes NHERF1 (also known as EBP50), NHERF2 (also known as E3KARP; TKA-1; SIP-1), NHERF3 (also known as CAP70; CLAMP; Napi-Cap-1; PDZD1) and NHERF4 (also known as IKEPP; PDZK2; Napi-Cap-2). NHERF1 and NHERF2 have tandem PDZ domains (PDZ1-2); NHERF3 and NHERF4 have four PDZ domains (PDZ1-4). NHERFs are involved in the regulation of multiple receptors or transporters, such as type II sodium-phosphate cotransporter (Npt2a), purinergic P2Y1 receptor P2Y1R, the beta2-adrenergic receptor (beta2-AR), parathyroid hormone receptor type 1 (PTHR), the lysophosphatidic acid receptors (LPARs), sodium-hydrogen exchanger 3 (NHE3), and cystic fibrosis transmembrane conductance regulator (CFTR). NHERF-PDZ1 domain interaction partners include Npt2a, purinergic P2Y1 receptor, beta2-AR, CFTR, PTHR, NH3, G-protein-coupled receptor kinase 6 (GRK6A), platelet-derived growth factor receptor (PDGFR), B1 subunit of the H+ATPase, cholesterol, receptor for activated C-kinase RACK1, aquaporin 9, among others. The NHERF PDZ2 domain interacts with fewer proteins: NHERF1 PDZ2 binds Npt2a, PTHR, beta-catenin, aquaporin 9, and RACK1; NHERF2 PDZ2 binds LPA2, P2Y1R, and NHE3, cGMP-dependent protein kinase type II (cGKII). NHERF4 PDZ1 and PDZ4 bind the epithelial Ca(2+) channels TRPV5 and TRPV6. NHERF2/NHERF3 heterodimerization is mediated by PDZ domains of NHERF2 and the C-terminal PDZ domain recognition motif of NHERF3. NHERF4 regulates several transporters mediating influx of xenobiotics and nutrients in the small intestine. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This NHERF-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467249 [Multi-domain]  Cd Length: 80  Bit Score: 43.97  E-value: 2.26e-05
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   18 VRLFKRKvGGLGFLVKERVSKPPVIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVDLSYDSALEVLRgiASETHVVLIL 97
Cdd:cd06768      3 CHLVKGP-EGYGFNLHAEKGRPGHFIREVDPGSPAERAGL-KDGDRLVEVNGENVEGESHEQVVEKIK--ASGNQVTLLV 78
COG4097 COG4097
Predicted ferric reductase [Inorganic ion transport and metabolism];
1209-1398 2.47e-05

Predicted ferric reductase [Inorganic ion transport and metabolism];


Pssm-ID: 443273 [Multi-domain]  Cd Length: 442  Bit Score: 48.74  E-value: 2.47e-05
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1209 YSISSSPDMyPDEVHLTVAIVSYHTRdgegpvhhgvcssWLNRIQADDVVpcFVRGaP--SFHLPRNPQVPC-ILVGPGT 1285
Cdd:COG4097    266 FSISSAPGG-DGRLRFTIKALGDFTR-------------RLGRLKPGTRV--YVEG-PygRFTFDRRDTAPRqVWIAGGI 328
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1286 GIAPFRSFWQqrqfDIQHKGMNPCPMVLVFGCRQSKiDHIYREE--TLQAKNKGVfrELYTAYSREPDRpkkyvqdVLQE 1363
Cdd:COG4097    329 GITPFLALLR----ALAARPGDQRPVDLFYCVRDEE-DAPFLEElrALAARLAGL--RLHLVVSDEDGR-------LTAE 394
                          170       180       190
                   ....*....|....*....|....*....|....*
gi 1958667836 1364 QLAESVyRALKEQggHIYVCGDVTMAADVLKAIQR 1398
Cdd:COG4097    395 RLRRLV-PDLAEA--DVFFCGPPGMMDALRRDLRA 426
PDZ1_PTPN13-like cd23072
PDZ domain 1 of protein tyrosine phosphatase non-receptor type 13 (PTPN13), and related ...
15-95 2.50e-05

PDZ domain 1 of protein tyrosine phosphatase non-receptor type 13 (PTPN13), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of PTPN13 [also known as Fas-associated protein-tyrosine phosphatase 1 (FAP-1), protein-tyrosine phosphatase 1E (PTP-E1), and protein-tyrosine phosphatase (PTPL1)], and related domains. PTPN13 regulates negative apoptotic signaling and mediates phosphoinositide 3-kinase (PI3K) signaling. PTPN13 has five PDZ domains. Proteins known to interact with PTPN13 PDZ domains include: PLEKHA1 and PLEKHA2 via PTPN13-PDZ domain 1, Fas receptor and thyroid receptor-interacting protein 6 via PTPN13-PDZ domain 2, nerve growth factor receptor and protein kinase N2 via PTPN13-PDZ domain 3, PDZ and LIM domain 4 (PDLIM4) via PTPN13-PDZ domains 2 and 4, and brain calpain-2 via PTPN13-PDZ domains 3, 4 and 5. Calpain-2-mediated PTPN13 fragments may be involved in abnormal tau aggregation and increased risk for Alzheimer's disease. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PTPN13 family PDZ1 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467285 [Multi-domain]  Cd Length: 92  Bit Score: 44.40  E-value: 2.50e-05
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   15 VISVRLFKRKVGGLGFLV----KERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASE 90
Cdd:cd23072      2 ITLVNLKKDAKYGLGFQIvggeKSGRLDLGIFISSITPGGPADLDGRLKPGDRLISVNDVSLEGLSHDAAVEILQNAPED 81

                   ....*
gi 1958667836   91 THVVL 95
Cdd:cd23072     82 VTLVV 86
PDZ3_Dlg1-2-4-like cd06795
PDZ domain 3 of human discs large homolog 1 (Dlg1), Dlg2, and Dlg4, Drosophila disc large (Dlg) ...
27-103 2.87e-05

PDZ domain 3 of human discs large homolog 1 (Dlg1), Dlg2, and Dlg4, Drosophila disc large (Dlg), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 3 of Drosophila Dlg1, human Dlg1, 2, and 4 and related domains. Dlg1 (also known as synapse-associated protein Dlg197; SAP-97), Dlg2 (also known as channel-associated protein of synapse-110; postsynaptic density protein 93, PSD-93), Dlg4 (also known as postsynaptic density protein 95, PSD-95; synapse-associated protein 90, SAP-90) each have 3 PDZ domains and belong to the membrane-associated guanylate kinase family. Dlg1 regulates antigen receptor signaling and cell polarity in lymphocytes, B-cell proliferation and antibody production, and TGFalpha bioavailability; its PDZ3 domain binds pro-TGFalpha, and its PDZ2 domain binds the TACE metalloprotease responsible for cleaving pro-TGFalpha to a soluble form. Dlg2 is involved in N-methyl-D-aspartate (NMDA) receptor signaling, regulating surface expression of NMDA receptors in dorsal horn neurons of the spinal cord; it interacts with NMDA receptor subunits and with Shaker-type K+ channel subunits to cluster into a channel complex. The Dlg4 PDZ1 domain binds NMDA receptors, and its PDZ2 domain binds neuronal nitric oxide synthase (nNOS), forming a complex in neurons. The Drosophila Scribble complex (Scribble, Dlg, and lethal giant larvae) plays a role in apico-basal cell polarity, and in other forms of polarity, including regulation of the actin cytoskeleton, cell signaling and vesicular trafficking, and in tumor development; postsynaptic targeting of Drosophila DLG requires interactions mediated by the first two PDZ domains. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Dlg-like family PDZ3 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467257 [Multi-domain]  Cd Length: 91  Bit Score: 44.27  E-value: 2.87e-05
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1958667836   27 GLGFLVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVVLILRgPEGF 103
Cdd:cd06795     13 GLGFNIVGGEDGEGIFISFILAGGPADLSGELRRGDQILSVNGVDLRNATHEQAAAALKNAGQTVTIIAQYK-PEEY 88
FNR_N-term_Iron_sulfur_binding cd06194
Iron-sulfur binding ferredoxin reductase (FNR) proteins combine the FAD and NAD(P) binding ...
1206-1388 3.08e-05

Iron-sulfur binding ferredoxin reductase (FNR) proteins combine the FAD and NAD(P) binding regions of FNR with an N-terminal Iron-Sulfur binding cluster domain. Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria in which they participate in a wide variety of redox metabolic pathways. The C-terminal domain contains most of the NADP(H) binding residues and the N-terminal domain interacts non-covalently with the isoalloxazine rings of the flavin molecule which lies largely in a large gap betweed the two domains. Ferredoxin-NADP+ reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2 which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99791 [Multi-domain]  Cd Length: 222  Bit Score: 46.88  E-value: 3.08e-05
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1206 PRYYSISSSPDMyPDEVHLtvaivsyHTRDgegpVHHGVCSSWL-NRIQADDVVPcfVRG--APSFHLPRNPQVPCILVG 1282
Cdd:cd06194     39 ARSYSPTSLPDG-DNELEF-------HIRR----KPNGAFSGWLgEEARPGHALR--LQGpfGQAFYRPEYGEGPLLLVG 104
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1283 PGTGIAPFRSFWQQrQFDIQHKGmnpcPMVLVFGCRQskIDHIYREETLQ--AKNKGVFRELYTAySREPDRPkkyvQDV 1360
Cdd:cd06194    105 AGTGLAPLWGIARA-ALRQGHQG----EIRLVHGARD--PDDLYLHPALLwlAREHPNFRYIPCV-SEGSQGD----PRV 172
                          170       180
                   ....*....|....*....|....*...
gi 1958667836 1361 LQEQLAESVYRALKEQggHIYVCGDVTM 1388
Cdd:cd06194    173 RAGRIAAHLPPLTRDD--VVYLCGAPSM 198
DegQ COG0265
Periplasmic serine protease, S1-C subfamily, contain C-terminal PDZ domain [Posttranslational ...
41-123 3.33e-05

Periplasmic serine protease, S1-C subfamily, contain C-terminal PDZ domain [Posttranslational modification, protein turnover, chaperones];


Pssm-ID: 440035 [Multi-domain]  Cd Length: 274  Bit Score: 47.45  E-value: 3.33e-05
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   41 VIISDLIRGGAAEQSGLiQAGDIILAVNDRPLvdlsyDSALEVLRGIAS----ETHVVLILRgpegftthlettftgDGT 116
Cdd:COG0265    203 VLVARVEPGSPAAKAGL-RPGDVILAVDGKPV-----TSARDLQRLLASlkpgDTVTLTVLR---------------GGK 261

                   ....*..
gi 1958667836  117 PKTIRVT 123
Cdd:COG0265    262 ELTVTVT 268
PDZ_MPP5-like cd06798
PDZ domain of membrane palmitoylated protein 5 (MPP5), Drosophila Stardust, and related ...
41-68 3.72e-05

PDZ domain of membrane palmitoylated protein 5 (MPP5), Drosophila Stardust, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of MPP5, Drosophila Stardust, and related domains. MPP5 (also known as MAGUK p55 subfamily member 1, protein associated with Lin-7 1 or PALS1) and Drosophila Stardust are membrane-associated guanylate kinase (MAGUK)-like proteins that serve as signaling and scaffolding proteins, linking different proteins critical to the formation and maintenance of tight junctions (TJ) and apical-basal polarity. Apical-basal polarity determinants cluster in complexes; in particular, the Crumbs complex (Crb, MPP5, and PATJ) and the PAR/aPKC-complex (PAR-3, PAR-6, aPKC) determine the apical plasma membrane domain. Within the Crumbs complex, Crb is stabilized in the plasma membrane by MPP5, which in turn recruits PATJ and Lin-7 to the complex. MPP5 also links the Crumbs complex with the PAR/aPKC-complex. The Drosophila homolog of the Crumbs complex is the (CRB)-Stardust (Sdt)-Discs Lost (Dlt) complex. MPP5 also acts as an interaction partner for SARS-CoV envelope protein E, which results in delayed formation of TJs and dysregulation of cell polarity. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MPP5-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467259 [Multi-domain]  Cd Length: 79  Bit Score: 43.49  E-value: 3.72e-05
                           10        20
                   ....*....|....*....|....*...
gi 1958667836   41 VIISDLIRGGAAEQSGLIQAGDIILAVN 68
Cdd:cd06798     23 VIISRIVKGGAAEKSGLLHEGDEILEIN 50
PDZ3_Scribble-like cd06702
PDZ domain 3 of Drosophila Scribble, human Scribble homolog, and related domains; PDZ (PSD-95 ...
35-98 3.84e-05

PDZ domain 3 of Drosophila Scribble, human Scribble homolog, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 2 of Drosophila Scribble (also known as LAP4), human Scribble homolog (also known as hScrib, LAP4, CriB1, ScrB1 and Vartul), and related domains. They belong to the LAP family, which describes proteins that contain either one or four PDZ domains and 16 LRRs (leucine-rich repeats) and function in controlling cell shape, size and subcellular protein localization. In Drosophila, the Scribble complex, comprising Scribble, discs large, and lethal giant larvae, plays a role in apico-basal cell polarity, in other forms of polarity, including regulation of the actin cytoskeleton, cell signaling and vesicular trafficking, and in tumor development. Mammalian Scribble is important in many aspects of cancer development. Scribble and its homologs can be downregulated or overexpressed in cancer; they have a role in cancer beyond their function in loss of cell polarity. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Scribble-like family PDZ3 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467186 [Multi-domain]  Cd Length: 89  Bit Score: 43.78  E-value: 3.84e-05
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gi 1958667836   35 RVSKPPVIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVDLSYDSALEVLrgIASETHVVLILR 98
Cdd:cd06702     28 GVDEPGIFISKVIPDGAAAKSGL-RIGDRILSVNGKDLRHATHQEAVSAL--LSPGQEIKLLVR 88
PDZ1_Scribble-like cd06704
PDZ domain 1 of Drosophila Scribble, human Scribble homolog, and related domains; PDZ (PSD-95 ...
23-98 3.89e-05

PDZ domain 1 of Drosophila Scribble, human Scribble homolog, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of Drosophila Scribble (also known as LAP4), human Scribble homolog (also known as hScrib, LAP4, CriB1, ScrB1 and Vartul), and related domains. They belong to the LAP family, which describes proteins that contain either one or four PDZ domains and 16 LRRs (leucine-rich repeats) and function in controlling cell shape, size and subcellular protein localization. In Drosophila, the Scribble complex, comprising Scribble, discs large, and lethal giant larvae, plays a role in apico-basal cell polarity, in other forms of polarity, including regulation of the actin cytoskeleton, cell signaling and vesicular trafficking, and in tumor development. Mammalian Scribble is important in many aspects of cancer development. Scribble and its homologs can be downregulated or overexpressed in cancer; they have a role in cancer beyond their function in loss of cell polarity. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Scribble-like family PDZ1 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467188 [Multi-domain]  Cd Length: 87  Bit Score: 43.81  E-value: 3.89e-05
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gi 1958667836   23 RKVGGLGFLVKERVSKPP-------VIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVDLSYDSALEVLRGiASETHVVL 95
Cdd:cd06704      7 RQTGGLGISIAGGKGSTPykgddegIFISRVTEGGPAAKAGV-RVGDKLLEVNGVDLVDADHHEAVEALKN-SGNTVTMV 84

                   ...
gi 1958667836   96 ILR 98
Cdd:cd06704     85 VLR 87
PDZ_MPP3-MPP4-MPP7-like cd06799
PDZ domain of membrane palmitoylated proteins 3 (MPP3), MPP4, and MPP7, and related domains; ...
18-84 5.06e-05

PDZ domain of membrane palmitoylated proteins 3 (MPP3), MPP4, and MPP7, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of MPP3, MPP4, and MPP7, and related domains. MPP3 (also known as MAGUK p55 subfamily member 3, erythrocyte membrane protein p55, or EMP55), MPP4 (also known as MAGUK p55 subfamily member 4 or Discs large homolog 6), and MPP7 (also known as MAGUK p55 subfamily member 7) are membrane-associated guanylate kinase (MAGUK)-like proteins. MPP3 is part of a cell adhesion protein complex including tumor suppressor CADM1 and actin-binding protein 4.1B. Participation in the Crumbs cell polarity complex has also been demonstrated for MPP7 in epithelial cells, and for MPP3 and MPP4 in the retina. MPP4 is needed for proper localization of plasma membrane calcium ATPases and maintenance of calcium homeostasis at the rod photoreceptor synaptic terminals. Binding partners of the MPP3 PDZ domain include nectin-3, serotonin 5-hydroxytryptamine, 5-HT(2C) receptor, and a cell adhesion protein, TSLC1 (tumor suppressor in lung cancer 1); fragments of MPP4 having the PDZ domain bind CRB (PDZ-SH3-GUK) and GABA transporter GAT1 (PDZ-SH3). PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MPP1-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467260 [Multi-domain]  Cd Length: 81  Bit Score: 43.00  E-value: 5.06e-05
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gi 1958667836   18 VRLFKRKvGGLGFLVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVL 84
Cdd:cd06799      3 VRLVKNN-EPLGATIKRDEKTGAIVVARIMRGGAADRSGLIHVGDELREVNGISVEGKDPEEVIQIL 68
PDZ5_INAD-like cd23066
PDZ domain 5 of inactivation no after potential D (INAD), and related domains; PDZ (PSD-95 ...
18-86 5.75e-05

PDZ domain 5 of inactivation no after potential D (INAD), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 5 of INAD, and related domains. INAD assembles key enzymes of the Drosophila compound eye photo-transduction pathway into a supramolecular complex, supporting efficient and fast light signaling. It contains 5 PDZ domains arranged in tandem (PDZ1-PDZ5) which independently bind various proteins. INAD PDZ2 binds eye-specific protein kinase C, INAD PDZ3 binds transient receptor potential (TRP) channel, and INAD PDZ45 tandem binds NORPA (phospholipase Cbeta, PLCbeta). Mutations of the inaD gene that lead to disruption of each of these interactions impair fly photo signal transduction. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This INAD-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467279 [Multi-domain]  Cd Length: 80  Bit Score: 42.88  E-value: 5.75e-05
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gi 1958667836   18 VRLFKR--KVGGLGFLVKERVSkppVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRG 86
Cdd:cd23066      2 VELMKKagKELGLSLSPNEGIG---CTIADLLPGGYAEIDGKLQKGDIITKFNGDALSGLPFQVCYALFKG 69
PDZ4_LNX1_2-like cd06680
PDZ domain 4 of human Ligand of Numb protein X 1 (LNX1) and LNX2, and related domains; PDZ ...
17-85 6.61e-05

PDZ domain 4 of human Ligand of Numb protein X 1 (LNX1) and LNX2, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 4 of LNX1 (also known as PDZ domain-containing RING finger protein 2, PDZRN2)and LNX2 (also known as PDZ domain-containing RING finger protein 1, PDZRN1), and related domains. LNX1 and LNX2 are Ring (Really Interesting New Gene) finger and PDZ domain-containing E3 ubiquitin ligases that bind to the cell fate determinant protein NUMB and mediate its ubiquitination. LNX1 can ubiquitinate a number of other ligands including PPFIA1, KLHL11, KIF7 and ERC2. LNX1 and LNX2 each have four PDZ domains. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This LNX family PDZ4 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467168 [Multi-domain]  Cd Length: 89  Bit Score: 43.10  E-value: 6.61e-05
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gi 1958667836   17 SVRLFKRKVGGLGFLV----KERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLR 85
Cdd:cd06680      2 DITLRRSSSGSLGFSIvggyEESHGNQPFFVKSIVPGTPAYNDGRLKCGDIILAVNGVSTVGMSHAALVPLLK 74
PDZ_Lin-7-like cd06796
PDZ domain of protein Lin-7 and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), ...
27-99 9.12e-05

PDZ domain of protein Lin-7 and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of Lin-7 (also known as LIN-7 or LIN7), and related domains. Lin-7 targets and organize protein complexes to epithelial and synaptic plasma membranes. There are three mammalian Lin-7 homologs: Lin-7A (protein lin-7 homolog A, also known as mammalian lin-seven protein 1 (MALS-1), vertebrate lin-7 homolog 1 (Veli-1), tax interaction protein 33); Lin-7B (also known as MALS-2, Veli-2); and Lin-7C (also known as MALS-3, Veli-3). Lin-7 is involved in localization of the Let-23 growth factor receptor to the basolateral membrane of epithelial cells, in tight junction localization of insulin receptor substrate p53 (IRSp53), in retaining gamma-aminobutyric (GABA) transporter (BGT-1) at the basolateral surface of epithelial cells, and in regulating recruitment of neurotransmitter receptors to the postsynaptic density (PSD). The Lin7 PDZ domain binds Let-23, BGT and beta-catenin, and NMDA (N-methyl-D-aspartate) receptor NR2B. Lin-7 also binds to the PDZ binding motif located in the C-terminal tail of Rhotekin, an effector protein for small GTPase Rho. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Lin-7-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467258 [Multi-domain]  Cd Length: 86  Bit Score: 42.42  E-value: 9.12e-05
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gi 1958667836   27 GLGFLV---KERVSkpPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRgiASETHVVLILRG 99
Cdd:cd06796     13 GLGFNVmggKEQNS--PIYISRIIPGGVADRHGGLKRGDQLLSVNGVSVEGEHHEKAVELLK--AAQGSVKLVVRY 84
PDZ4_MAGI-1_3-like cd06734
PDZ domain 4 of membrane-associated guanylate kinase inverted 1 (MAGI-1), MAGI-2, and MAGI-3, ...
18-95 9.45e-05

PDZ domain 4 of membrane-associated guanylate kinase inverted 1 (MAGI-1), MAGI-2, and MAGI-3, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 4 of MAGI1, 2, 3 (MAGI is also known as Membrane-associated guanylate kinase, WW and PDZ domain-containing protein) and related domains. MAGI proteins have been implicated in the control of cell migration and invasion through altering the activity of phosphatase and tensin homolog (PTEN) and modulating Akt signaling. Four MAGI proteins have been identified (MAGI1-3 and MAGIX). MAGI1-3 have 6 PDZ domains and bind to the C-terminus of PTEN via their PDZ2 domain. MAGIX has a single PDZ domain that is related to MAGI1-3 PDZ domain 5. Other binding partners for MAGI1 include JAM4, C-terminal tail of high risk HPV-18 E6, megalin, TRAF6, Kir4.1 (basolateral K+ channel subunit), and cadherin 23; for MAGI2, include DASM1, dendrin, axin, beta- and delta-catenin, neuroligin, hyperpolarization-activated cation channels, beta1-adrenergic receptors, NMDA receptor, and TARPs; and for MAGI3 includes LPA2. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MAGI family PDZ4 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2); arranged as beta-strands A, -B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467216 [Multi-domain]  Cd Length: 84  Bit Score: 42.60  E-value: 9.45e-05
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gi 1958667836   18 VRLFKRKVGGLGF-LVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRgiASETHVVL 95
Cdd:cd06734      4 VTLTRRENEGFGFvIISSVNKKSGSKIGRIIPGSPADRCGQLKVGDRILAVNGISILNLSHGDIVNLIK--DSGLSVTL 80
PDZ10_MUPP1-PDZ8_PATJ-like cd06673
PDZ domain 10 of multi-PDZ-domain protein 1 (MUPP1), domain 8 of PATJ (protein-associated ...
41-98 1.08e-04

PDZ domain 10 of multi-PDZ-domain protein 1 (MUPP1), domain 8 of PATJ (protein-associated tight junction) and similar domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 10 of MUPP1, PDZ domain 8 of PATJ, and related domains. MUPP1 and PATJ serve as scaffolding proteins linking different proteins and protein complexes involved in the organization of tight junctions and epithelial polarity. MUPP1 contains an L27 (Lin-2 and Lin-7 binding) domain and 13 PDZ domains. PATJ (also known as INAD-like) contains an L27 domain and ten PDZ domains. MUPP1 and PATJ share several binding partners, including junctional adhesion molecules (JAM), zonula occludens (ZO)-3, Pals1 (protein associated with Lin-7), Par (partitioning defective)-6 proteins, and nectins (adherence junction adhesion molecules). PATJ lacks 3 PDZ domains seen in MUPP1: PDZ6, 9, and 13; consequently, MUPP1 PDZ7 and 8 align with PATJ PDZ6 and 7; and MUPP1 PDZ domains 10-12 align with PATJ PDZ domains 8-10. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MUPP1-like family PDZ10 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467161 [Multi-domain]  Cd Length: 86  Bit Score: 42.28  E-value: 1.08e-04
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gi 1958667836   41 VIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHvVLILR 98
Cdd:cd06673     30 IIIHEVYEDGAAAKDGRLWAGDQILEVNGEDLRKATHDEAINVLRQTPQKVR-LLVYR 86
PDZ4_Scribble-like cd06701
PDZ domain 4 of Drosophila Scribble, human Scribble homolog, and related domains; PDZ (PSD-95 ...
41-95 1.25e-04

PDZ domain 4 of Drosophila Scribble, human Scribble homolog, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 4 of Drosophila Scribble (also known as LAP4), human Scribble homolog (also known as hScrib, LAP4, CriB1, ScrB1 and Vartul), and related domains. They belong to the LAP family, which describes proteins that contain either one or four PDZ domains and 16 LRRs (leucine-rich repeats) and function in controlling cell shape, size and subcellular protein localization. In Drosophila, the Scribble complex, comprising Scribble, discs large, and lethal giant larvae, plays a role in apico-basal cell polarity, in other forms of polarity, including regulation of the actin cytoskeleton, cell signaling and vesicular trafficking, and in tumor development. Mammalian Scribble is important in many aspects of cancer development. Scribble and its homologs can be downregulated or overexpressed in cancer; they have a role in cancer beyond their function in loss of cell polarity. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Scribble-like family PDZ4 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467185 [Multi-domain]  Cd Length: 98  Bit Score: 42.60  E-value: 1.25e-04
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gi 1958667836   41 VIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVVL 95
Cdd:cd06701     40 IFISKINPDGAAARDGRLKVGQRILEVNGQSLLGATHQEAVRILRSVGDTLTLLV 94
RseP COG0750
Membrane-associated protease RseP, regulator of RpoE activity [Posttranslational modification, ...
39-123 1.40e-04

Membrane-associated protease RseP, regulator of RpoE activity [Posttranslational modification, protein turnover, chaperones, Transcription];


Pssm-ID: 440513 [Multi-domain]  Cd Length: 349  Bit Score: 45.85  E-value: 1.40e-04
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gi 1958667836   39 PPVIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVdlSYDSALEVLRGIASETHVVLILRgpegftthlettftgDGTPK 118
Cdd:COG0750    128 TPPVVGEVVPGSPAAKAGL-QPGDRIVAINGQPVT--SWDDLVDIIRASPGKPLTLTVER---------------DGEEL 189

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gi 1958667836  119 TIRVT 123
Cdd:COG0750    190 TLTVT 194
PDZ1_GRIP1-2-like cd06687
PDZ domain 1 of glutamate receptor-interacting protein 1 (GRIP1) and GRIP2, and related ...
18-95 1.43e-04

PDZ domain 1 of glutamate receptor-interacting protein 1 (GRIP1) and GRIP2, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of alpha-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptor (AMPAR) binding proteins GRIP1 (ABP/GRIP2) and GRIP2, and related domains. GRIP1 and GRIP2 each have 7 PDZ domains. The interaction of GRIP1 and GRIP2 with GluA2/3 (AMPAR subunit) regulates AMPAR trafficking and synaptic targeting. GRIP1 has an essential role in regulating AMPAR trafficking during synaptic plasticity and learning and memory. GRIP1 and GRIP2 interact with a variety of other proteins associated with protein trafficking and internalization, for example GRIP1 also interacts with KIF5 (also known as kinesin 1), EphB receptors, scaffold protein liprin-alpha, and the rasGEF GRASP-1. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This GRIP family PDZ1 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467175 [Multi-domain]  Cd Length: 83  Bit Score: 42.01  E-value: 1.43e-04
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gi 1958667836   18 VRLFKRKVGGLGFLVK---ERVSKPPViiSDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASEthVV 94
Cdd:cd06687      3 VELIKKEGSTLGLTVSggiDKDGKPRV--SNLRPGGIAARSDQLNVGDYIKSVNGIRTTKLRHDEIISLLKNVGER--VV 78

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gi 1958667836   95 L 95
Cdd:cd06687     79 L 79
PDZ3_PDZD2-PDZ1_hPro-IL-16-like cd06759
PDZ domain 3 of PDZ domain containing 2 (PDZD2), PDZ domain 1 of human pro-interleukin-16 ...
49-98 1.66e-04

PDZ domain 3 of PDZ domain containing 2 (PDZD2), PDZ domain 1 of human pro-interleukin-16 (isoform 1, 1332 AA), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 3 of PDZD2, also known as KIAA0300, PIN-1, activated in prostate cancer (AIPC) and PDZ domain-containing protein 3 (PDZK3). PDZD2 has seven PDZ domains. PDZD2 is expressed at exceptionally high levels in the pancreas and certain cancer tissues, such as prostate cancer. It promotes the proliferation of insulinoma cells and is upregulated during prostate tumorigenesis. In osteosarcoma (OS), the microRNA miR-363 acts as a tumor suppressor by inhibiting PDZD2. This family also includes the first PDZ domain (PDZ1) of human pro-interleukin-16 (isoform 1, also known as nPro-Il-16; 1332 amino-acid protein). Precursor IL-16 is cleaved to produce pro-IL-16 and mature IL-16 (derived from the C-terminal 121 AA). Pro-IL-16 functions as a regulator of T cell growth; mature IL-16 is a CD4 ligand that induces chemotaxis and CD25 expression in CD4+ T cells. IL-16 bioactivity has been closely associated with the progression of several different cancers. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PDZD2-like family PDZ3 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467240 [Multi-domain]  Cd Length: 87  Bit Score: 41.88  E-value: 1.66e-04
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gi 1958667836   49 GGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASEThVVLILR 98
Cdd:cd06759     39 GGAAAEDGRLKEGDEILEVNGESLQGLTHQEAIQKFKQIKKGL-VVLTVR 87
PDZ_FRMPD1_3_4-like cd06769
PDZ domain of FERM and PDZ domain-containing protein 1 (FRMPD1), FRMPD3, FRMPD4, and related ...
17-85 1.66e-04

PDZ domain of FERM and PDZ domain-containing protein 1 (FRMPD1), FRMPD3, FRMPD4, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of FRMPD1, FRMPD3, FRMPD4, and related domains. FRMPD1 (also known as FERM domain-containing protein 2, FRMD2), inhibits the malignant phenotype of lung cancer by activating the Hippo pathway via interaction with WWC3; the FRMPD1 PDZ domain binds WWC3. FRMPD3 is a target gene of the neuron-specific transcription factor NPAS4 that is involved in synaptic plasticity. FRMPD4 (also known as PDZ domain-containing protein 10, PDZD10, PDZK10, PSD-95-interacting regulator of spine morphogenesis, and Preso) regulates dendritic spine morphogenesis, and mGluR1/5 signaling; the FRMPD4 PDZ domain binds PAK-interacting exchange factor-beta (betaPix). PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This FRMPD1,3,4-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467250 [Multi-domain]  Cd Length: 75  Bit Score: 41.46  E-value: 1.66e-04
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....
gi 1958667836   17 SVRLFKRKVGGLGFLVKervSKPPVIISDLIRGGAAEqsGLIQAGDIILAVNDRPLVDLSYDSALEVLR 85
Cdd:cd06769      1 TVEIQRDAVLGFGFVAG---SERPVVVRSVTPGGPSE--GKLLPGDQILKINNEPVEDLPRERVIDLIR 64
PDZ_SYNJ2BP-like cd06709
PDZ domain of synaptojanin-2-binding protein (SYNJ2BP), and related domains; PDZ (PSD-95 ...
22-92 1.85e-04

PDZ domain of synaptojanin-2-binding protein (SYNJ2BP), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of SYNJ2BP, and related domains. SYNJ2BP (also known as mitochondrial outer membrane protein 25, OMP25) regulates endocytosis of activin type 2 receptor kinases through the Ral/RALBP1-dependent pathway and may be involved in suppression of activin-induced signal transduction. Binding partners of the SYNJ2BP PDZ domain include activin type II receptors (ActR-II), and SYNJ2. SYNJ2BP interacts with the PDZ binding motif of the Notch Delta-like ligand 1 (DLL1) and DLL4, promoting Delta-Notch signaling, and inhibiting sprouting angiogenesis. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This SYNJ2BP-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467193 [Multi-domain]  Cd Length: 86  Bit Score: 41.51  E-value: 1.85e-04
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1958667836   22 KRKVGGLGFLVKERVSKP------PVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETH 92
Cdd:cd06709      6 KRGPSGLGFNIVGGTDQPyipndsGIYVAKIKEDGAAAIDGRLQEGDKILEINGQSLENLTHQDAVELFRNAGEDVK 82
PDZ1_FRMPD2-like cd23071
PDZ domain 1 of FERM and PDZ domain-containing protein 2 (FRMPD2), and related domains; PDZ ...
15-102 2.07e-04

PDZ domain 1 of FERM and PDZ domain-containing protein 2 (FRMPD2), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of FRMPD2 (also known as PDZ domain-containing protein 4, and related domains. FRMPD2 is localized in the basolateral membranes of polarized epithelial cells and is associated with tight junction formation and immune response; it contains 3 PDZ domains. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PTPN13 family PDZ1 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467284 [Multi-domain]  Cd Length: 92  Bit Score: 41.71  E-value: 2.07e-04
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   15 VISVRLFKRKVGGLGFLV--KERVSK--PPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGiaSE 90
Cdd:cd23071      2 IVCVTLKRDPKRGFGFVIvgGENTGKldLGIFIASIIPGGPAEKDGRIKPGGRLISLNNISLEGVTFNTAVKILQN--SP 79
                           90
                   ....*....|..
gi 1958667836   91 THVVLILRGPEG 102
Cdd:cd23071     80 DEVELIISQPKD 91
PDZ_rhophilin-like cd06712
PDZ domain of rhophilin-1, rhophilin-2, and related domains; PDZ (PSD-95 (Postsynaptic density ...
21-71 2.56e-04

PDZ domain of rhophilin-1, rhophilin-2, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of rhophilin-1, rhophilin-2, and related domains. Rhophilin-1 (RHPN1, also known as GTP-Rho-binding protein 1) and rhophilin-2 (RHPN2, also known as GTP-Rho-binding protein 2) are Rho-GTP binding proteins involved in cytoskeletal dynamics. Rhophilin-2 inhibits RhoA's activity to induce F-actin stress fibers. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This rhophilin-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467196 [Multi-domain]  Cd Length: 78  Bit Score: 41.03  E-value: 2.56e-04
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1958667836   21 FKRKVGGLGFLVKervSKPPVIISDLIRGGAAEQSGLiQAGDIILAVNDRP 71
Cdd:cd06712      6 LTKEEGGFGFTLR---GDSPVQVASVDPGSCAAEAGL-KEGDYIVSVGGVD 52
cpPDZ_Deg_HtrA-like cd06779
permuted PDZ domain of Deg/high-temperature requirement factor A (HtrA) family of housekeeping ...
41-104 2.62e-04

permuted PDZ domain of Deg/high-temperature requirement factor A (HtrA) family of housekeeping serine proteases and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of Deg/HtrA-type serine proteases that participate in folding and degradation of aberrant proteins, and in processing and maturation of native proteins. Typically, these proteases have an N-terminal serine protease domain and at least one C-terminal PDZ domain that recognizes substrates, and in some cases activates the protease function. An exception is yeast Nma11p which has two protease domains and four PDZ domains; its N-terminal half is comprised of a protease domain, followed by two PDZ domains, and its C-terminal half has a similar domain arrangement. HtrA-type proteases include the human HtrA1-4 and MBTPS2, tricorn protease, DegS, DegP and C-terminal processing peptidase, cyanobacterial serine proteases Hhoa, HhoB, and HtrA, and yeast Nma11p. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-termini of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains and as well as those with circular permutations and domain swapping of beta-strands. The canonical PDZ domain contains six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2); arranged as A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F. This Deg/HtrA family PDZ domain is a circularly permuted PDZ domain which places beta-strand A at the C-terminus. Another permutation exists in the PDZ superfamily which places both beta-strands A and B on the C-terminus.


Pssm-ID: 467621 [Multi-domain]  Cd Length: 91  Bit Score: 41.51  E-value: 2.62e-04
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*
gi 1958667836   41 VIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVdlSYDSALEVLRGIASETHVVL-ILRGPEGFT 104
Cdd:cd06779     27 VLVAEVIPGSPAAKAGL-KEGDVILSVNGKPVT--SFNDLRAALDTKKPGDSLNLtILRDGKTLT 88
PRK09004 PRK09004
FMN-binding protein MioC; Provisional
893-945 2.65e-04

FMN-binding protein MioC; Provisional


Pssm-ID: 181608 [Multi-domain]  Cd Length: 146  Bit Score: 42.90  E-value: 2.65e-04
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*...
gi 1958667836  893 GDGPD----LRDNFESTGP-LANVRFSVFGLGSRAYPHFCAFGHAVDTLLEELGGERI 945
Cdd:PRK09004    60 GDLPDnlqpFFEELQEQKPdLSQVRFAAIGIGSSEYDTFCGAIDKLEQLLKAKGAKQI 117
PDZ_GOPC-like cd06800
PDZ domain of Golgi-associated PDZ and coiled-coil motif-containing protein (GOPC), and ...
16-84 2.68e-04

PDZ domain of Golgi-associated PDZ and coiled-coil motif-containing protein (GOPC), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of GOPC and related domains. GOPC, also known as PIST (PDZ domain protein interacting specifically with TC10), FIG (fused in glioblastoma), and CAL (CFTR-associated ligand), regulates the trafficking of a wide array of proteins, including small GTPases, receptors, and cell surface molecules such as cadherin 23 and CFTR. It may regulate CFTR chloride currents and acid-sensing ASIC3 currents by modulating cell surface expression of both channels, and may play a role in autophagy. Interaction partners of the GOPC PDZ domains include: FZD5, FZD8, ASIC3, CFTR, MUC3, ARFRP1, Ggamma13, neuroligin, and Stargazin. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This GOPC-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467261 [Multi-domain]  Cd Length: 83  Bit Score: 41.20  E-value: 2.68e-04
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|..
gi 1958667836   16 ISVRLFKRKVGGLGFLV---KERvsKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVL 84
Cdd:cd06800      1 RKVLLSKEPHEGLGISItggKEH--GVPILISEIHEGQPADRCGGLYVGDAILSVNGIDLRDAKHKEAVTIL 70
PDZ_RGS12-like cd06710
PDZ domain of regulator of G-protein signaling 12 (RGS12), and related domains; PDZ (PSD-95 ...
27-93 2.75e-04

PDZ domain of regulator of G-protein signaling 12 (RGS12), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of RGS12, and related domains. RGS12 downregulates GPCR signal transduction by increasing the GTPase activity of G-protein alpha subunits, thereby driving G-proteins into their inactive GDP-bound form. The RGS12 PDZ domain can bind selectively to C-terminal (A/S)-T-X-(L/V) motifs as found within both the CXCR2 IL-8 receptor, and the alternative 3' exon form of RGS12. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This RGS12-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467194 [Multi-domain]  Cd Length: 76  Bit Score: 40.69  E-value: 2.75e-04
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1958667836   27 GLGFLVKervSKPPVIISDLIRGGAAEQSGLiQAGDIILAVNDrplVDLSYDSALEVLRGIASETHV 93
Cdd:cd06710     11 GYGFTIS---GQAPCVLSCVVRGSPADVAGL-KAGDQILAVNG---INVSKASHEDVVKLIGKCTGV 70
PDZ2_GRIP1-2-like cd06681
PDZ domain 2 of glutamate receptor-interacting protein 1 (GRIP1) and GRIP2, and related ...
15-91 2.84e-04

PDZ domain 2 of glutamate receptor-interacting protein 1 (GRIP1) and GRIP2, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of alpha-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptor (AMPAR) binding proteins GRIP1 (ABP/GRIP2) and GRIP2, and related domains. GRIP1 and GRIP2 each have 7 PDZ domains. The interaction of GRIP1 and GRIP2 with GluA2/3 (AMPAR subunit) regulates AMPAR trafficking and synaptic targeting. GRIP1 has an essential role in regulating AMPAR trafficking during synaptic plasticity and learning and memory. GRIP1 and GRIP2 interact with a variety of other proteins associated with protein trafficking and internalization, for example GRIP1 also interacts with KIF5 (also known as kinesin 1), EphB receptors, scaffold protein liprin-alpha, and the rasGEF GRASP-1. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This GRIP family PDZ2 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467169 [Multi-domain]  Cd Length: 89  Bit Score: 41.06  E-value: 2.84e-04
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   15 VISVRLfKRKVGGLGFLV-----KERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIAS 89
Cdd:cd06681      2 TVEVTL-EKEGNSFGFVIrggahEDRNKSRPLTVTHVRPGGPADREGTIKPGDRLLSVDGISLHGATHAEAMSILKQCGQ 80

                   ..
gi 1958667836   90 ET 91
Cdd:cd06681     81 EA 82
PDZ2_MUPP1-like cd06667
PDZ domain 2 of multi-PDZ-domain protein 1 (MUPP1) and PATJ (protein-associated tight junction) ...
26-96 3.03e-04

PDZ domain 2 of multi-PDZ-domain protein 1 (MUPP1) and PATJ (protein-associated tight junction) and similar domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 2 of MUPP1 and PATJ, and related domains. MUPP1 and PATJ serve as scaffolding proteins linking different proteins and protein complexes involved in the organization of tight junctions and epithelial polarity. MUPP1 contains an L27 (Lin-2 and Lin-7 binding) domain and 13 PDZ domains. PATJ (also known as INAD-like) contains an L27 domain and ten PDZ domains. MUPP1 and PATJ share several binding partners, including junctional adhesion molecules (JAM), zonula occludens (ZO)-3, Pals1 (protein associated with Lin-7), Par (partitioning defective)-6 proteins, and nectins (adherence junction adhesion molecules). PATJ lacks 3 PDZ domains seen in MUPP1: PDZ6, 9, and 13; consequently, MUPP1 PDZ7 and 8 align with PATJ PDZ6 and 7; and MUPP1 PDZ domains 10-12 align with PATJ PDZ domains 8-10. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MUPP1-like family PDZ2 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F


Pssm-ID: 467155 [Multi-domain]  Cd Length: 80  Bit Score: 40.73  E-value: 3.03e-04
                           10        20        30        40        50        60        70
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gi 1958667836   26 GGLGF-LVKERVSKppVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGiaSETHVVLI 96
Cdd:cd06667     10 SGLGFgIVGGKSTG--VVVKTILPGGVADRDGRLRSGDHILQIGDTNLRGMGSEQVAQVLRQ--CGSHVRLV 77
PDZ2_L-delphilin-like cd06744
PDZ domain 2 of delphilin (L-delphilin isoform), and related domains; PDZ (PSD-95 ...
17-86 3.36e-04

PDZ domain 2 of delphilin (L-delphilin isoform), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 2 of delphilin (also known as glutamate receptor, ionotropic, delta 2-interacting protein 1, L-delphilin). Delphilin, a postsynaptic protein which it is selectively expressed at cerebellar Purkinje cells, links the glutamate receptor delta 2 subunit (GluRdelta2) with the actin cytoskeleton and various signaling molecules. Two alternatively spliced isoforms of delphilin have been characterized: L-delphilin has two PDZ domains, PDZ1 and PDZ2, and S-delphilin has a single PDZ domain (PDZ2). These two isoforms are differently palmitoylated and may be involved in controlling GluRdelta2 signaling in Purkinje cells. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This delphilin-like family PDZ2 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F


Pssm-ID: 467226 [Multi-domain]  Cd Length: 75  Bit Score: 40.72  E-value: 3.36e-04
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   17 SVRLfKRKVGGLGFLVKervSKPPVIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVDLSYDSALEVLRG 86
Cdd:cd06744      1 TVRV-YRGNGSFGFTLR---GHAPVYIESVDPGSAAERAGL-KPGDRILFLNGLDVRNCSHDKVVSLLQG 65
COG3975 COG3975
Predicted metalloprotease, contains C-terminal PDZ domain [General function prediction only];
28-145 3.44e-04

Predicted metalloprotease, contains C-terminal PDZ domain [General function prediction only];


Pssm-ID: 443174 [Multi-domain]  Cd Length: 591  Bit Score: 45.20  E-value: 3.44e-04
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   28 LGFLVKERVSKppVIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVDLSYDSALEVLRgiASETHVVLILRgpegftthl 107
Cdd:COG3975    485 LGLRVSADGGG--LVVTSVLWGSPAYKAGL-SAGDELLAIDGLRVTADNLDDALAAYK--PGDPIELLVFR--------- 550
                           90       100       110
                   ....*....|....*....|....*....|....*...
gi 1958667836  108 ettftgDGTPKTIRVTqPLGPPTKAVDLSHQPSASKDQ 145
Cdd:COG3975    551 ------RDELRTVTVT-LAAAPADTYKLERVEGATPAQ 581
PDZ1_PTPN13_FRMPD2-like cd06694
PDZ domain 1 of protein tyrosine phosphatase non-receptor type 13 (PTPN13),FERM and PDZ ...
18-85 3.59e-04

PDZ domain 1 of protein tyrosine phosphatase non-receptor type 13 (PTPN13),FERM and PDZ domain-containing protein 2 (FRMPD2), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of PTPN13 [also known as Fas-associated protein-tyrosine phosphatase 1 (FAP-1), protein-tyrosine phosphatase 1E (PTP-E1), and protein-tyrosine phosphatase (PTPL1)], FRMPD2 (also known as PDZ domain-containing protein 4; PDZ domain-containing protein 5C), and related domains. PTPN13 regulates negative apoptotic signaling and mediates phosphoinositide 3-kinase (PI3K) signaling. PTPN13 has five PDZ domains. Proteins known to interact with PTPN13 PDZ domains include: PLEKHA1 and PLEKHA2 via PTPN13-PDZ domain 1, Fas receptor and thyroid receptor-interacting protein 6 via PTPN13-PDZ domain 2, nerve growth factor receptor and protein kinase N2 via PTPN13-PDZ domain 3, PDZ and LIM domain 4 (PDLIM4) via PTPN13-PDZ domains 2 and 4, and brain calpain-2 via PTPN13-PDZ domains 3, 4 and 5. Calpain-2-mediated PTPN13 fragments may be involved in abnormal tau aggregation and increased risk for Alzheimer's disease. FRMPD2 is localized in the basolateral membranes of polarized epithelial cells and is associated with tight junction formation and immune response; it contains 3 PDZ domains. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PTPN13 family PDZ1 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467180 [Multi-domain]  Cd Length: 92  Bit Score: 41.23  E-value: 3.59e-04
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|..
gi 1958667836   18 VRLFKRKVGGLGFLV----KERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLR 85
Cdd:cd06694      5 VTLKKDPQKGLGFTIvggeNSGSLDLGIFVKSIIPGGPADKDGRIKPGDRIIAINGQSLEGKTHHAAVEIIQ 76
PDZ_Radil-like cd06690
PDZ domain of Ras-associating and dilute domain-containing protein (Radil) and related domains; ...
39-86 4.13e-04

PDZ domain of Ras-associating and dilute domain-containing protein (Radil) and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of Radil (also known as protein KIAA1849) and related domains. Radil is required for cell adhesion and migration of neural crest precursors during development. Radil is a component of a Rasip1-Radil-ARHGAP29 complex at endothelial cell-cell junctions. Rap1, via its effectors Radil and Rasip1 and their binding partner ArhGAP29, controls the endothelial barrier by decreasing Rho-mediated radial tension on cell-cell junctions. ArhGAP29 binds the Radil PDZ domain. The Radil PDZ domain also binds kinesin family protein 14 (KIF14); KIF14 negatively regulates Rap1-mediated inside-out integrin activation by tethering Radil on microtubules. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Radil-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467177 [Multi-domain]  Cd Length: 88  Bit Score: 40.74  E-value: 4.13e-04
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*...
gi 1958667836   39 PPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRG 86
Cdd:cd06690     30 PGIYIRTLVPDSPAARDGRLRLGDRILAVNGTSLVGADYQSAMDLIRT 77
PDZ2_FL-whirlin cd06741
PDZ domain 2 of the full-length isoform of whirlin and related domains; PDZ (PSD-95 ...
46-98 5.02e-04

PDZ domain 2 of the full-length isoform of whirlin and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 2 of the full-length isoform of whirlin and related domains. Whirlin is an essential protein for developmental pathways in photoreceptor cells of the retina and hair cells of the inner ear. The full-length whirlin isoform has two harmonin N-like domains, three PDZ domains, a proline-rich region, and a PDZ-binding motif. Whirlin isoforms may form different complexes at the periciliary membrane complex (PMC) in photoreceptors, and the stereociliary tip and base in inner ear hair cells. It interacts with ADGRV1 and usherin at the PMC; with SANS and RpgrORF15 at the connecting cilium in photoreceptors; with EPS8, MYO15A, p55, and CASK proteins at the stereociliary tip of inner ear hair cells; and with ADGRV1, usherin, and PDZD7 at the stereociliary base in inner ear hair cells. Mutations in the gene encoding whirlin (WHRN; also known as USH2D and DFNB31), have been found to cause either USH2 subtype (USH2D) or autosomal recessive non-syndromic deafness type 31 (DFNB31). Whirlin is the key protein in the USH2 complex (whirlin, usherin and GPR98) which recruits other USH2 causative proteins at the periciliary membrane in photoreceptors and the ankle link of the stereocilia in hair cells. Whirlin's interaction with espin, another stereociliary protein, may be important for the architecture of the USH2 complex. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This whirlin family PDZ2 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467223 [Multi-domain]  Cd Length: 84  Bit Score: 40.32  E-value: 5.02e-04
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....
gi 1958667836   46 LIRGG----------------AAEQSGLiQAGDIILAVNDRPLVDLSYDSALEVLRgiaSETHVVLILR 98
Cdd:cd06741     17 MIRGGaeyglgiyvtgvdpgsVAENAGL-KVGDQILEVNGRSFLDITHDEAVKILK---SSKHLIMTVK 81
PDZ3_FL-whirlin-like cd06742
PDZ domain 3 of the full-length isoform of whirlin, PDZ domain 1 of the short isoform of ...
48-88 8.75e-04

PDZ domain 3 of the full-length isoform of whirlin, PDZ domain 1 of the short isoform of whirlin, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 3 of the full-length isoform of whirlin, PDZ domain 1 of the short isoform of whirlin, and related domains. Whirlin is an essential protein for developmental pathways in photoreceptor cells of the retina and hair cells of the inner ear. The full-length whirlin isoform has two harmonin N-like domains, three PDZ domains, a proline-rich region, and a PDZ-binding motif. Whirlin isoforms may form different complexes at the periciliary membrane complex (PMC) in photoreceptors, and the stereociliary tip and base in inner ear hair cells. It interacts with ADGRV1 and usherin at the PMC; with SANS and RpgrORF15 at the connecting cilium in photoreceptors; with EPS8, MYO15A, p55, and CASK proteins at the stereociliary tip of inner ear hair cells; and with ADGRV1, usherin, and PDZD7 at the stereociliary base in inner ear hair cells. Mutations in the gene encoding whirlin (WHRN; also known as USH2D and DFNB31), have been found to cause either USH2 subtype (USH2D) or autosomal recessive non-syndromic deafness type 31 (DFNB31). Whirlin is the key protein in the USH2 complex (whirlin, usherin and GPR98) which recruits other USH2 causative proteins at the periciliary membrane in photoreceptors and the ankle link of the stereocilia in hair cells. Whirlin's interaction with espin, another stereociliary protein, may be important for the architecture of the USH2 complex. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This whirlin family PDZ3 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F


Pssm-ID: 467224 [Multi-domain]  Cd Length: 91  Bit Score: 40.03  E-value: 8.75e-04
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|.
gi 1958667836   48 RGGAAEQSGLIQAGDIILAVNDRPLVDLSYDsalEVLRGIA 88
Cdd:cd06742     35 RGGSAHNCGGLKVGHVILEVNGTSLRGLEHR---EAARLIA 72
oxygenase_e_transfer_subunit cd06213
The oxygenase reductase FAD/NADH binding domain acts as part of the multi-component bacterial ...
1206-1395 9.23e-04

The oxygenase reductase FAD/NADH binding domain acts as part of the multi-component bacterial oxygenases which oxidize hydrocarbons. Electron transfer is from NADH via FAD (in the oxygenase reductase) and an [2FE-2S] ferredoxin center (fused to the FAD/NADH domain and/or discrete) to the oxygenase. Dioxygenases add both atoms of oxygen to the substrate while mono-oxygenases add one atom to the substrate and one atom to water. In dioxygenases, Class I enzymes are 2 component, containing a reductase with Rieske type [2Fe-2S] redox centers and an oxygenase. Class II are 3 component, having discrete flavin and ferredoxin proteins and an oxygenase. Class III have 2 [2Fe-2S] centers, one fused to the flavin domain and the other separate.


Pssm-ID: 99809  Cd Length: 227  Bit Score: 42.68  E-value: 9.23e-04
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1206 PRYYSISSSPDmyPDevhltvAIVSYHTRDgegpVHHGVCSSWL---NRIQAddvvPCFVRGA-PSFHLpRNPQVPCILV 1281
Cdd:cd06213     44 ARSYSFANAPQ--GD------GQLSFHIRK----VPGGAFSGWLfgaDRTGE----RLTVRGPfGDFWL-RPGDAPILCI 106
                           90       100       110       120       130       140       150       160
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gi 1958667836 1282 GPGTGIAPFRSFWQQRQFDIQHKgmnpcPMVLVFGCRQS----KIDHIyreETLQAKNKGVFReLYTAYSREP-DRPKKY 1356
Cdd:cd06213    107 AGGSGLAPILAILEQARAAGTKR-----DVTLLFGARTQrdlyALDEI---AAIAARWRGRFR-FIPVLSEEPaDSSWKG 177
                          170       180       190       200
                   ....*....|....*....|....*....|....*....|..
gi 1958667836 1357 VQDVLQEQLAEsvyraLKEQGGHIYVCGDVTM---AADVLKA 1395
Cdd:cd06213    178 ARGLVTEHIAE-----VLLAATEAYLCGPPAMidaAIAVLRA 214
cyt_b5_reduct_like cd06183
Cytochrome b5 reductase catalyzes the reduction of 2 molecules of cytochrome b5 using NADH as ...
1243-1409 1.05e-03

Cytochrome b5 reductase catalyzes the reduction of 2 molecules of cytochrome b5 using NADH as an electron donor. Like ferredoxin reductases, these proteins have an N-terminal FAD binding subdomain and a C-terminal NADH binding subdomain, separated by a cleft, which accepts FAD. The NADH-binding moiety interacts with part of the FAD and resembles a Rossmann fold. However, NAD is bound differently than in canonical Rossmann fold proteins. Nitrate reductases, flavoproteins similar to pyridine nucleotide cytochrome reductases, catalyze the reduction of nitrate to nitrite. The enzyme can be divided into three functional fragments that bind the cofactors molybdopterin, heme-iron, and FAD/NADH.


Pssm-ID: 99780 [Multi-domain]  Cd Length: 234  Bit Score: 42.55  E-value: 1.05e-03
                           10        20        30        40        50        60        70        80
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gi 1958667836 1243 GVCSSWLNRIQADDVVpcFVRGA-PSFHLPRNPQVPCI-LVGPGTGIAPFRSFWQQRQFDIQHKGmnpcPMVLVFGCRqs 1320
Cdd:cd06183     72 GKMSQYLHSLKPGDTV--EIRGPfGKFEYKPNGKVKHIgMIAGGTGITPMLQLIRAILKDPEDKT----KISLLYANR-- 143
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1321 KIDHI-YREE--TLQAKNKGVFRELYTAySREPDRPKKYV----QDVLQEQLAESvyralKEQGGHIYVCGDVTMaadVL 1393
Cdd:cd06183    144 TEEDIlLREEldELAKKHPDRFKVHYVL-SRPPEGWKGGVgfitKEMIKEHLPPP-----PSEDTLVLVCGPPPM---IE 214
                          170
                   ....*....|....*.
gi 1958667836 1394 KAIQRIMTQQGKLSEE 1409
Cdd:cd06183    215 GAVKGLLKELGYKKDN 230
FldA COG0716
Flavodoxin [Energy production and conversion]; Flavodoxin is part of the Pathway/BioSystem: ...
755-821 1.08e-03

Flavodoxin [Energy production and conversion]; Flavodoxin is part of the Pathway/BioSystem: Heme biosynthesis


Pssm-ID: 440480 [Multi-domain]  Cd Length: 135  Bit Score: 40.66  E-value: 1.08e-03
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1958667836  755 ATILYATETGKSQAYAKTLCEIFKhAFDAKAMSMEEYDIVHLEHEALVLVVTSTFGnGDPPENGEKF 821
Cdd:COG0716      1 ILIVYGSTTGNTEKVAEAIAEALG-AAGVDLFEIEDADLDDLEDYDLLILGTPTWA-GELPDDWEDF 65
PDZ1_hSTXBP4-PDZ2_GgSTXBP4-like cd06698
PDZ1 domain of human syntaxin-binding protein 4 (STXBP4), PDZ2 domain of Gallus gallus ...
24-84 1.09e-03

PDZ1 domain of human syntaxin-binding protein 4 (STXBP4), PDZ2 domain of Gallus gallus uncharacterized STXBP4 isoform X1, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of human syntaxin-binding protein 4 (STXBP4), PDZ2 domain of Gallus gallus uncharacterized STXBP4 isoform X1, and related domains. Human STXBP4 (also known as Synip) includes a single PDZ domain, a coiled-coil domain, and a WW domain (named for its two conserved tryptophans); Gallus gallus STXBP4 isoform X1 contains 2 PDZ domains (PDZ1 and PDZ2). Human STXBP4 plays a role in the translocation of transport vesicles from the cytoplasm to the plasma membrane: insulin induces the dissociation of the STXBP4 and STX4 complex liberating STX4 to interact with Vamp2, and to form the SNARE complex thereby promoting vesicle fusion. It may also play a role in the regulation of insulin release by pancreatic beta cells after stimulation by glucose. Human STXBP4 is also known to physically associate with a prominent isoform of TP63 (deltaNp63alpha 9) whose overexpression promotes squamous cell carcinoma development, and in doing so prevents degradation of this isoform by the Cdc20-APC/C complex, Itch, and RACK1. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This STXBP4-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467184 [Multi-domain]  Cd Length: 89  Bit Score: 39.60  E-value: 1.09e-03
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gi 1958667836   24 KVGGLGFLVK---ERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVL 84
Cdd:cd06698      9 KSTGLGLSIVggiNRPEGPMVFIQEVIPGGDCYKDGRLRPGDQLVSINKESLIGVTLEEAKSIL 72
PDZ2_LNX1_2-like cd06678
PDZ domain 2 of human Ligand of Numb protein X 1 (LNX1) and LNX2, and related domains; PDZ ...
16-98 1.34e-03

PDZ domain 2 of human Ligand of Numb protein X 1 (LNX1) and LNX2, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 2 of LNX1 (also known as PDZ domain-containing RING finger protein 2, PDZRN2) and LNX2 (also known as PDZ domain-containing RING finger protein 1, PDZRN1), and related domains. LNX1 and LNX2 are Ring (Really Interesting New Gene) finger and PDZ domain-containing E3 ubiquitin ligases that bind to the cell fate determinant protein NUMB and mediate its ubiquitination. LNX1 can ubiquitinate a number of other ligands including PPFIA1, KLHL11, KIF7 and ERC2. LNX1 and LNX2 each have four PDZ domains. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This LNX family PDZ2 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467166 [Multi-domain]  Cd Length: 82  Bit Score: 39.15  E-value: 1.34e-03
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gi 1958667836   16 ISVRLFKRKVGGLGFLVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVVl 95
Cdd:cd06678      1 LHVTLNKRDGEQLGIKLVRKKDEPGVFILDLLEGGLAARDGRLKSDDRVLAINGQDLRHGTPEQAAQIIQASGERVHFV- 79

                   ...
gi 1958667836   96 ILR 98
Cdd:cd06678     80 VSR 82
cpPDZ1_DegP-like cd10839
circularly permuted first PDZ domain (PDZ1) of Escherichia coli periplasmic serine ...
41-76 1.53e-03

circularly permuted first PDZ domain (PDZ1) of Escherichia coli periplasmic serine endoprotease DegP and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of Escherichia coli DegP (also known as heat shock protein DegP and Protease Do) and related domains. DegP belongs to the HtrA family of housekeeping proteases. It acts as a protease, degrading transiently denatured and unfolded or misfolded proteins which accumulate in the periplasm following heat shock or other stress conditions, and as a molecular chaperone at low temperatures. DegP has two PDZ domains in addition to the protease domain; its PDZ1 domain is responsible for identifying the distinct substrate sequences that affect degradation (degron) of the substrate sequence, and its PDZ2 domain is responsible for combining with other DegP monomers to form a stable oligomer structure. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains and as well as those with circular permutations and domain swapping of beta-strands. The canonical PDZ domain contains six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2); arranged as A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F. This DegP family PDZ domain 1 is a circularly permuted PDZ domain which places beta-strand A on the C-terminus. Another permutation exists in the PDZ superfamily which places both beta-strands A and B on the C-terminus.


Pssm-ID: 467630 [Multi-domain]  Cd Length: 91  Bit Score: 39.00  E-value: 1.53e-03
                           10        20        30
                   ....*....|....*....|....*....|....*.
gi 1958667836   41 VIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVDLS 76
Cdd:cd10839     27 ALVAQVLPDSPAAKAGL-KAGDVILSLNGKPITSSA 61
PDZ4_PTPN13-like cd06696
PDZ domain 4 of protein tyrosine phosphatase non-receptor type 13 (PTPN13), and related ...
16-95 1.62e-03

PDZ domain 4 of protein tyrosine phosphatase non-receptor type 13 (PTPN13), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 4 of PTPN13 [also known as Fas-associated protein-tyrosine phosphatase 1 (FAP-1), protein-tyrosine phosphatase 1E (PTP-E1), and protein-tyrosine phosphatase (PTPL1)] and related domains. PTPN13 regulates negative apoptotic signaling and mediates phosphoinositide 3-kinase (PI3K) signaling. PTPN13 has five PDZ domains. Proteins known to interact with PTPN13 PDZ domains include: PLEKHA1 and PLEKHA2 via PTPN13-PDZ domain 1, Fas receptor and thyroid receptor-interacting protein 6 via PTPN13-PDZ domain 2, nerve growth factor receptor and protein kinase N2 via PTPN13-PDZ domain 3, PDZ and LIM domain 4 (PDLIM4) via PTPN13-PDZ domains 2 and 4, and brain calpain-2 via PTPN13-PDZ domains 3, 4 and 5. Calpain-2-mediated PTPN13 fragments may be involved in abnormal tau aggregation and increased risk for Alzheimer's disease. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PTPN13 family PDZ4 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467182 [Multi-domain]  Cd Length: 85  Bit Score: 38.83  E-value: 1.62e-03
                           10        20        30        40        50        60        70        80
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gi 1958667836   16 ISVRLFKRKVGGLGFLVKERVSKPPVIISDLIRGgAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGIASETHVVL 95
Cdd:cd06696      4 LEVTLTKSEKGSLGFTVTKGKDDNGCYIHDIVQD-PAKSDGRLRPGDRLIMVNGVDVTNMSHTEAVSLLRAAPKEVTLVL 82
PDZ_PDLIM-like cd06753
PDZ domain of PDZ-LIM family proteins, and related domains; PDZ (PSD-95 (Postsynaptic density ...
40-95 1.67e-03

PDZ domain of PDZ-LIM family proteins, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of PDZ-LIM family proteins including PDLIM1-7, and related domains. PDZ-LIM family proteins (also known as Zasp PDZ domain proteins) are involved in the rearrangement of the actin cytoskeleton; they mediate association with the cytoskeleton through alpha-actinin as well as with other proteins involved in signal transduction pathways. Members of this family include PDLIM1 (also known as C-terminal LIM domain protein 1, elfin, LIM domain protein CLP-36), PDLIM2 (also known as PDZ-LIM protein mystique), PDLIM3 (also known as actinin-associated LIM protein, alpha-actinin-2-associated LIM protein, ALP), PDLIM4 (also known as LIM protein RIL, Reversion-induced LIM protein), PDLIM5 (also known as enigma homolog, ENH, enigma-like PDZ and LIM domains protein), PDLIM6 (also known as LIM domain-binding protein 3, ZASP, Cypher, Oracle), and PDLIM7 (also known as PDZ and LIM domain protein 7, LIM mineralization protein, LMP; protein enigma). PDLIM1 has been shown to negatively regulate NF-kappaB-mediated signaling in the cytoplasm. PDLIM7 negatively regulates p53 through binding murine double minute 2 (MDM2). The PDZ domains of PDZ-LIM family proteins PDLIM1, 2, 3, 5, 6, 7 have been shown to bind actin. Other PDZ-LIM family PDZ domain binding partners include thyroid receptor interacting protein-6 (PDLIM4-PDZ), the LIM domain of PDLIM4 (PDLIM4-PDZ), tropomyosin (PDLIM7-PDZ), myotilin and calsarcin 1 (PDLIM6-PDZ), and proteins from the myotilin and FATZ (calsarcin/myozenin) families (PDLIM1, 3, 4, 6 PDZ domains). PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This PDLIM-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467235 [Multi-domain]  Cd Length: 79  Bit Score: 38.67  E-value: 1.67e-03
                           10        20        30        40        50
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gi 1958667836   40 PVIISDLIRGGAAEQSGLIQaGDIILAVNDRPLVDLSYDSALEVLRGIASETHVVL 95
Cdd:cd06753     23 PLTISRVTPGGKAAQANLRP-GDVILAINGESTEGMTHLEAQNKIKAATGSLSLTL 77
FNR_iron_sulfur_binding_1 cd06215
Iron-sulfur binding ferredoxin reductase (FNR) proteins combine the FAD and NAD(P) binding ...
1207-1390 1.69e-03

Iron-sulfur binding ferredoxin reductase (FNR) proteins combine the FAD and NAD(P) binding regions of FNR with an iron-sulfur binding cluster domain. Ferredoxin-NADP+ (oxido)reductase is an FAD-containing enzyme that catalyzes the reversible electron transfer between NADP(H) and electron carrier proteins such as ferredoxin and flavodoxin. Isoforms of these flavoproteins (i.e. having a non-covalently bound FAD as a prosthetic group) are present in chloroplasts, mitochondria, and bacteria in which they participate in a wide variety of redox metabolic pathways. The C-terminal portion of the FAD/NAD binding domain contains most of the NADP(H) binding residues and the N-terminal sub-domain interacts non-covalently with the isoalloxazine rings of the flavin molecule which lies largely in a large gap betweed the two domains. In this ferredoxin like sub-group, the FAD/NAD sub-domains is typically fused to a C-terminal iron-sulfur binding domain. Iron-sulfur proteins play an important role in electron transfer processes and in various enzymatic reactions. The family includes plant and algal ferredoxins which act as electron carriers in photosynthesis and ferredoxins which participate in redox chains from bacteria to mammals. Ferredoxin reductase first accepts one electron from reduced ferredoxin to form a flavin semiquinone intermediate. The enzyme then accepts a second electron to form FADH2 which then transfers two electrons and a proton to NADP+ to form NADPH.


Pssm-ID: 99811 [Multi-domain]  Cd Length: 231  Bit Score: 41.81  E-value: 1.69e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1207 RYYSISSSPDMyPDEVHLTVAIVsyhtrdgEGpvhhGVCSSWLN-------RIQADDvvpcfVRGApsFHLPRNPQVPCI 1279
Cdd:cd06215     47 RAYTLSSSPSR-PDSLSITVKRV-------PG----GLVSNWLHdnlkvgdELWASG-----PAGE--FTLIDHPADKLL 107
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1280 LVGPGTGIAPFRS---FWQQRQFDIQhkgmnpcpMVLVFGCRqSKIDHIYREE--TLQAKNKGvFRELYTAYSREPDRPK 1354
Cdd:cd06215    108 LLSAGSGITPMMSmarWLLDTRPDAD--------IVFIHSAR-SPADIIFADEleELARRHPN-FRLHLILEQPAPGAWG 177
                          170       180       190
                   ....*....|....*....|....*....|....*..
gi 1958667836 1355 KYVQDVLQEQLAeSVYRALKEQggHIYVCG-DVTMAA 1390
Cdd:cd06215    178 GYRGRLNAELLA-LLVPDLKER--TVFVCGpAGFMKA 211
PDZ_shroom2_3_4-like cd06750
PDZ domain of shroom2, shroom3, shroom4, and related domains; PDZ (PSD-95 (Postsynaptic ...
40-98 1.75e-03

PDZ domain of shroom2, shroom3, shroom4, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of shroom2, shroom3, shroom4, and related domains. Shroom family proteins shroom2 (also known as apical-like protein; protein APXL), shroom3 (also known as shroom-related protein), and shroom4 (also known as second homolog of apical protein) are essential regulators of cell morphology during animal development; they regulate cell architecture by directing the subcellular distribution and activation of Rho kinase (ROCK), which results in the localized activation of non-muscle myosin. The interaction between shroom and ROCK is mediated by the shroom domain 2 (SD2). PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This shroom2,3,4-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged as beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467232 [Multi-domain]  Cd Length: 82  Bit Score: 38.86  E-value: 1.75e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*....
gi 1958667836   40 PVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLvDLSYDSALEVLRGiaSETHVVLILR 98
Cdd:cd06750     26 PLVISKIEEGGKAASVGKLQVGDEVVNINGVPL-SGSRQEAIQLVKG--SHKTLKLVVR 81
PDZ1_FL-whirlin cd06740
PDZ domain 1 of the full-length isoform of whirlin and related domains; PDZ (PSD-95 ...
47-86 1.94e-03

PDZ domain 1 of the full-length isoform of whirlin and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of the full-length isoform of whirlin and related domains. Whirlin is an essential protein for developmental pathways in photoreceptor cells of the retina and hair cells of the inner ear. The full-length whirlin isoform has two harmonin N-like domains, three PDZ domains, a proline-rich region, and a PDZ-binding motif. Whirlin isoforms may form different complexes at the periciliary membrane complex (PMC) in photoreceptors, and the stereociliary tip and base in inner ear hair cells. It interacts with ADGRV1 and usherin at the PMC; with SANS and RpgrORF15 at the connecting cilium in photoreceptors; with EPS8, MYO15A, p55, and CASK proteins at the stereociliary tip of inner ear hair cells; and with ADGRV1, usherin, and PDZD7 at the stereociliary base in inner ear hair cells. Mutations in the gene encoding whirlin (WHRN; also known as USH2D and DFNB31), have been found to cause either USH2 subtype (USH2D) or autosomal recessive non-syndromic deafness type 31 (DFNB31). Whirlin is the key protein in the USH2 complex (whirlin, usherin and GPR98) which recruits other USH2 causative proteins at the periciliary membrane in photoreceptors and the ankle link of the stereocilia in hair cells. Whirlin's interaction with espin, another stereociliary protein, may be important for the architecture of the USH2 complex. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This whirlin family PDZ1 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467222 [Multi-domain]  Cd Length: 82  Bit Score: 38.50  E-value: 1.94e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*.
gi 1958667836   47 IRGGA----------------AEQSGLiQAGDIILAVNDRPLVDLSYDSALEVLRG 86
Cdd:cd06740     19 IRGGAehgvgiyvslvepgslAEKEGL-RVGDQILRVNDVSFEKVTHAEAVKILRV 73
flavin_oxioreductase cd06189
NAD(P)H dependent flavin oxidoreductases use flavin as a substrate in mediating electron ...
1207-1408 2.01e-03

NAD(P)H dependent flavin oxidoreductases use flavin as a substrate in mediating electron transfer from iron complexes or iron proteins. Structurally similar to ferredoxin reductases, but with only 15% sequence identity, flavin reductases reduce FAD, FMN, or riboflavin via NAD(P)H. Flavin is used as a substrate, rather than a tightly bound prosthetic group as in flavoenzymes; weaker binding is due to the absence of a binding site for the AMP moeity of FAD.


Pssm-ID: 99786 [Multi-domain]  Cd Length: 224  Bit Score: 41.38  E-value: 2.01e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1207 RYYSISSSPDMyPDEVHLtvaivsyHTRDGEGpvhhGVCSS-WLNRIQADDVVPcfVRGaP--SFHLPRNPQVPCILVGP 1283
Cdd:cd06189     42 RPFSIASAPHE-DGEIEL-------HIRAVPG----GSFSDyVFEELKENGLVR--IEG-PlgDFFLREDSDRPLILIAG 106
                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836 1284 GTGIAPFRSFWQqrqfDIQHKGMNPcPMVLVFGCRQSKiDHIYRE--ETLQAKNKGVFrelYTA-YSREPDRPKK---YV 1357
Cdd:cd06189    107 GTGFAPIKSILE----HLLAQGSKR-PIHLYWGARTEE-DLYLDEllEAWAEAHPNFT---YVPvLSEPEEGWQGrtgLV 177
                          170       180       190       200       210
                   ....*....|....*....|....*....|....*....|....*....|.
gi 1958667836 1358 QDVLQEQLAEsvyraLKEQggHIYVCGDVTMAadvlKAIQRIMTQQGKLSE 1408
Cdd:cd06189    178 HEAVLEDFPD-----LSDF--DVYACGSPEMV----YAARDDFVEKGLPEE 217
cpPDZ_HtrA-like cd06785
circularly permuted PDZ domain of high-temperature requirement factor A (HtrA) family serine ...
41-101 2.19e-03

circularly permuted PDZ domain of high-temperature requirement factor A (HtrA) family serine proteases and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of HtrA family serine proteases including human HtrA1, HtrA2 (mitochondrial), HtrA3, and HtrA4, and related domains. These proteases are key enzymes associated with pregnancy. Their diverse biological functions include cell growth proliferation, migration and apoptosis. They are also implicated in disorders including Alzheimer's, Parkinson's, arthritis and cancer. HtrA1 (also known as high-temperature requirement A serine peptidase 1, L56, and serine protease 11) substrates include extracellular matrix proteins, proteoglycans, and insulin-like growth factor (IGF)-binding proteins. HtrA1 also inhibits signaling by members of the transforming growth factor beta (TGF-beta) family. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping of beta-strands. The canonical PDZ domain contains six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2); arranged as A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F. This HtrA-like PDZ domain is a circularly permuted PDZ domain which places beta-strand A on the C-terminus. Another permutation exists in the PDZ superfamily which places both beta-strands A and B on the C-terminus.


Pssm-ID: 467624 [Multi-domain]  Cd Length: 98  Bit Score: 39.02  E-value: 2.19e-03
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|..
gi 1958667836   41 VIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVdlsydSALEVLRGI-ASETHVVLILRGPE 101
Cdd:cd06785     33 VYVHKVIPGSPAQRAGL-KDGDVIISINGKPVK-----SSSDVYEAVkSGSSLLVVVRRGNE 88
PDZ6_MUPP1-like cd06670
PDZ domain 6 of multi-PDZ-domain protein 1 (MUPP1) and related domains; PDZ (PSD-95 ...
41-85 2.53e-03

PDZ domain 6 of multi-PDZ-domain protein 1 (MUPP1) and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 6 of multi-PDZ-domain protein 1 (MUPP1). MUPP1 and PATJ serve as scaffolding proteins linking different proteins and protein complexes involved in the organization of tight junctions and epithelial polarity. MUPP1 contains an L27 (Lin-2 and Lin-7 binding) domain and 13 PDZ domains. PATJ (also known as INAD-like) contains an L27 domain and ten PDZ domains. PATJ lacks 3 PDZ domains seen in MUPP1: PDZ6, PDZ9, and PDZ13. This MuPP1-like PDZ6 domain is therefore absent from PATJ. MUPP1 and PATJ share several binding partners, including junctional adhesion molecules (JAM), zonula occludens (ZO)-3, Pals1 (protein associated with Lin-7), Par (partitioning defective)-6 proteins, and nectins (adherence junction adhesion molecules). PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This MUPP1-like family PDZ6 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F


Pssm-ID: 467158 [Multi-domain]  Cd Length: 87  Bit Score: 38.39  E-value: 2.53e-03
                           10        20        30        40
                   ....*....|....*....|....*....|....*....|....*
gi 1958667836   41 VIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLR 85
Cdd:cd06670     29 CIVKSIIHGGAVSRDGRISVGDFIVSINNESLRNVTNAQARAILR 73
Peptidase_M50 pfam02163
Peptidase family M50;
40-116 2.88e-03

Peptidase family M50;


Pssm-ID: 426630 [Multi-domain]  Cd Length: 291  Bit Score: 41.32  E-value: 2.88e-03
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1958667836   40 PVIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVdlSYDSALEVLRGIASETHVVLILRGPEGFTTHLETTFTGDGT 116
Cdd:pfam02163   94 PPVIGGVAPGSPAAKAGL-KPGDVILSINGKKIT--SWQDLVEALAKSPGKPITLTVERGGQTLTVTITPKSSEESK 167
PDZ_ARHGEF11-12-like cd23069
PDZ domain of ARHGEF11, ARHGEF12, and related domains; PDZ (PSD-95 (Postsynaptic density ...
27-97 2.89e-03

PDZ domain of ARHGEF11, ARHGEF12, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of ARHGEF11, ARHGEF12, and related domains. This subfamily includes the GEFs (guanine exchange factors) ARHGEF11 (Rho guanine nucleotide exchange factor 11, known as PDZ-RhoGEF) and ARHGEF12 (Rho guanine nucleotide exchange factor 12, also known as leukemia-associated RhoGEF). GEFs activate Rho GTPases by promoting GTP binding. ARHGEF11/12 are regulators of G protein signaling (RGS) domain-containing GEFs; the RGS domain mediates their binding to and activation of Galpha (and Gq also in the case of ARHGEF12), in response to G-protein coupled receptor activation. ARHGEF11 and 12 are involved in serum-signaling, and regulate Yes-Associated Protein (YAP1)-dependent transcription. The ARHGEF12 PDZ domain binds plexin-B1 and the receptor tyrosine kinase insulin-like growth factor receptor (IGF-R1) beta-subunit. ARHGEF12 also interacts with glutamate receptor delta-1(GluD1), a postsynaptic organizer of inhibitory synapses in cortical pyramidal neurons. The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This ARHGEF11-12-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467282 [Multi-domain]  Cd Length: 76  Bit Score: 38.14  E-value: 2.89e-03
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|.
gi 1958667836   27 GLGFLVKervSKPPVIISDLIRGGAAEQSGlIQAGDIILAVNDRpLVDLSydSALEVLRGIASETHVVLIL 97
Cdd:cd23069     12 GYGLTVS---GDNPVFVQSVKEGGAAYRAG-VQEGDRIIKVNGT-LVTHS--NHLEVVKLIKSGSYVALTL 75
degP_htrA_DO TIGR02037
periplasmic serine protease, Do/DeqQ family; This family consists of a set proteins various ...
41-155 2.91e-03

periplasmic serine protease, Do/DeqQ family; This family consists of a set proteins various designated DegP, heat shock protein HtrA, and protease DO. The ortholog in Pseudomonas aeruginosa is designated MucD and is found in an operon that controls mucoid phenotype. This family also includes the DegQ (HhoA) paralog in E. coli which can rescue a DegP mutant, but not the smaller DegS paralog, which cannot. Members of this family are located in the periplasm and have separable functions as both protease and chaperone. Members have a trypsin domain and two copies of a PDZ domain. This protein protects bacteria from thermal and other stresses and may be important for the survival of bacterial pathogens.// The chaperone function is dominant at low temperatures, whereas the proteolytic activity is turned on at elevated temperatures. [Protein fate, Protein folding and stabilization, Protein fate, Degradation of proteins, peptides, and glycopeptides]


Pssm-ID: 273938 [Multi-domain]  Cd Length: 428  Bit Score: 41.82  E-value: 2.91e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   41 VIISDLIRGGAAEQSGLiQAGDIILAVNDRPLvdlsyDSALEVLRGIAS----ETHVVLILRgpegftthlettftgDGT 116
Cdd:TIGR02037  259 ALVAQVLPGSPAEKAGL-KAGDVITSVNGKPI-----SSFADLRRAIGTlkpgKKVTLGILR---------------KGK 317
                           90       100       110
                   ....*....|....*....|....*....|....*....
gi 1958667836  117 PKTIRVTqplgpptkavdLSHQPSASKDQSLAVDRVTGL 155
Cdd:TIGR02037  318 EKTITVT-----------LGASPEEQASSSNPFLGLTVA 345
cpPDZ_EcRseP-like cd23081
circularly permuted PDZ domains of Escherichia coli Regulator of sigma-E protease (RseP) and ...
41-123 3.47e-03

circularly permuted PDZ domains of Escherichia coli Regulator of sigma-E protease (RseP) and related domains; Permuted PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of ResP (also known as Site-2 protease RseP, and YaeL), and related domains. RseP is involved in the regulation of an extracytoplasmic stress response through the cleavage of membrane-spanning anti-stress-response transcription factor (anti-sigmE) protein RseA; it cleaves the peptide bond between the critical alanine and cysteine in the transmembrane region of RseA, releasing the cytoplasmic domain of RseA with its associated sigmaE. RseP contains two tandem-arranged periplasmic PDZ domains (PDZ-N/PDZ1 and PDZ-C/PDZ2) which act to negatively regulate protease action on intact RseA; they serve as a size-exclusion filter which prevents the access of an intact RseA into the active site of RseP. PDZ domains usually bind in sequence-specific manner to short peptide sequences located at the C-terminal of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains and as well as those with circular permutations and domain swapping of beta-strands. The canonical PDZ domain contains six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2); arranged as beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F. This RseP family PDZ domain is a circularly permuted PDZ domain which places both beta-strands A and B at the C-terminus. Another permutation exists in the PDZ superfamily which places beta-strand A at the C-terminus.


Pssm-ID: 467638 [Multi-domain]  Cd Length: 83  Bit Score: 37.94  E-value: 3.47e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   41 VIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVDLsYDSALEVLRGIASETHVVlILRgpegftthlettftgDGTPKTI 120
Cdd:cd23081      1 PVVGEVVANSPAAEAGL-KPGDRILKIDGQKVRTW-EDIVRIVRENPGKPLTLK-IER---------------DGKILTV 62

                   ...
gi 1958667836  121 RVT 123
Cdd:cd23081     63 TVT 65
PDZ_SIPA1-like cd06745
PDZ domain of signal-induced proliferation-associated protein 1 (SIPA1), and related domains; ...
20-96 3.85e-03

PDZ domain of signal-induced proliferation-associated protein 1 (SIPA1), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of SIPA1, and related domains. The Rap-GTPase activating protein SIPA1 (also known as GTPase-activating protein Spa-1, p130 SPA1) is a metastasis promoter; a polymorphism in a region of the Sipa1 gene encoding the PDZ domain is associated with metastasis. The SIPA1 PDZ domain binds ribosomal RNA processing 1 homolog B (Rrp1b). SIPA1 also forms a complex with water channel aquaporin-2 (AQP2) and plays a role in trafficking of AQP2, targeted positioning of which strictly regulates body water homeostasis; the SIPA1 PDZ domain binds AQP2. Rrp1b or AQP2 binding inhibits the RapGAP activity of SIPA1. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This SIPA1-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged as beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta- strand F.


Pssm-ID: 467227 [Multi-domain]  Cd Length: 73  Bit Score: 37.64  E-value: 3.85e-03
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1958667836   20 LFKRKVGGLGFLVKERVskppvIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVDLSYDSALEVLRGiASETHVVLI 96
Cdd:cd06745      4 LRRNGLGQLGFHVNYEG-----FVTEVERFGFAWQAGL-RQGSRLVEICKVPVATLTHEQMIDLLRT-SVKVKVTVI 73
PDZ1_Par3-like cd06691
PDZ domain 1 of partitioning defective 3 (Par3), and related domains; PDZ (PSD-95 ...
48-85 4.23e-03

PDZ domain 1 of partitioning defective 3 (Par3), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 1 of Par3 (or PAR3 or Par-3, also known as Atypical PKC isotype-specific-interacting protein, ASIP) and related domains; Drosophila bazooka PDZ1 belongs to a different PDZ family. Par3 is a scaffold protein involved in organizing cell polarity across animals. Par3 binds numerous molecules both for its recruitment to one pole of the cell and for downstream contributions to polarized cell function. It regulates cell polarity by targeting the Par complex proteins Par6 and atypical protein kinase C (aPKC) to specific cortical sites. Physical interactions between Par3 and the Par complex include: Par-3 PDZ domain 1 binding to the Par6 PDZ domain, Par3 PDZ domain 1 and PDZ domain 3 binding the Par6's PDZ-binding motif, and an interaction with an undefined region of aPKC that requires both Par3 PDZ2 and PDZ3. The PDZ domains of Par3 have also been implicated as potential phosphoinositide signaling integrators, since its second PDZ domain binds to phosphoinositides, and the third PDZ interacts with phosphoinositide phosphatase PTEN. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Par3 family PDZ1 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467178 [Multi-domain]  Cd Length: 98  Bit Score: 37.98  E-value: 4.23e-03
                           10        20        30
                   ....*....|....*....|....*....|....*...
gi 1958667836   48 RGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLR 85
Cdd:cd06691     42 EGSRAERDGRFQENDCIVEINGVDLIDKSFEQAQDIFR 79
PDZ_ZASP52-like cd23068
PDZ domain of Drosophila melanogaster PDZ and LIM domain protein Zasp52 (also known as Zasp), ...
23-85 4.61e-03

PDZ domain of Drosophila melanogaster PDZ and LIM domain protein Zasp52 (also known as Zasp), and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of Drosophila melanogaster Zasp52 and related domains. Drosophila melanogaster Zasp52 (also known as Z band alternatively spliced PDZ-motif protein or Zasp) colocalizes with integrins at myotendinous junctions and with alpha-actinin at Z-disks and is required for muscle attachment as well as Z-disk assembly and maintenance. The Zasp52 actin-binding site includes the extended PDZ domain and the ZM region. The Zasp52-PDZ domain is required for myofibril assembly. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This Zasp52-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467281 [Multi-domain]  Cd Length: 82  Bit Score: 37.51  E-value: 4.61e-03
                           10        20        30        40        50        60
                   ....*....|....*....|....*....|....*....|....*....|....*....|...
gi 1958667836   23 RKVGGLGFlvkervsKPPVIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVDLSYDSALEVLR 85
Cdd:cd23068     16 RLQGGADF-------GQPLSIQKVNPGSPADKAGL-RRGDVILRINGTDTSNLTHKQAQDLIK 70
PDZ2_harmonin cd06738
PDZ domain 2 of harmonin isoforms a, b, and c, and related domains; PDZ (PSD-95 (Postsynaptic ...
16-98 4.63e-03

PDZ domain 2 of harmonin isoforms a, b, and c, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 2 of harmonin isoforms a, b, and c, and related domains. Harmonin (also known as Usher Type 1C, PDZ-73 and AIE-75) is a key organizer of the Usher (USH) protein interactome. USH syndrome is the leading cause of hereditary sensory deaf-blindness in humans; three clinically distinct types of USH have been identified, type 1 to 3. The gene encoding harmonin (USH1C) is the causative gene for the USH type 1C phenotype. There are at least 10 alternatively spliced isoforms of harmonin, which are divided into three subclasses (a, b, and c). All isoforms contain the first two PDZ domains and the first coiled-coil domain. The a and b isoforms all have a third PDZ domain. The different PDZ domains are responsible for interactions with all known Usher syndrome type 1 proteins, and most Usher syndrome type 2 proteins. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This harmonin family PDZ2 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467220 [Multi-domain]  Cd Length: 82  Bit Score: 37.68  E-value: 4.63e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   16 ISVRLFKRKVGGLGF---LVKERVSKPPVIISDLIRGGAAEQSGLiQAGDIILAVNDRPLVDLSYDSALEVLRgiaSETH 92
Cdd:cd06738      1 KEKKVFISLVGTRGLgcsISSGPTQKPGIFISNVKPGSLAEEVGL-EVGDQIVEVNGTSFTNVDHKEAVMALK---SSRH 76

                   ....*.
gi 1958667836   93 VVLILR 98
Cdd:cd06738     77 LTITVR 82
PDZ_RIM-like cd06714
PDZ domain of Rab3-interacting molecule 1 (RIM), RIM2, piccolo and related domains; PDZ ...
42-98 4.83e-03

PDZ domain of Rab3-interacting molecule 1 (RIM), RIM2, piccolo and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of RIM, RIM2, piccolo and related domains. RIM proteins and Gallus gallus protein piccolo (also called aczonin) are involved in neurotransmitter release at presynaptic active zones, the site of vesicle fusion. A protein complex containing RIM proteins positions synaptic vesicles containing synaptotagmin at the active zone. RIM proteins simultaneously activate docking and priming of synaptic vesicles and recruit Ca2+-channels to active zones, thereby connecting primed synaptic vesicles to Ca2+-channels. RIM binding to vesicular Rab proteins (Rab3 and Rab27 isoforms) mediates vesicle docking; RIM binding to Munc13 activates vesicle priming; RIM binding to the Ca2+-channel, both directly and indirectly via RIM-BP, recruits the Ca2+-channels. The RIM PDZ domain interacts with the C-termini of N- and P/Q-type voltage-gated Ca2+-channels. RIM1, RIM2 and piccolo also participate in regulated exocytosis through binding cAMP-GEFII (cAMP-binding protein-guanidine nucleotide exchange factor II). The piccolo PDZ domain binds cAMP-GEFII. RIM2 also plays a role in dendrite formation by melanocytes. Caenorhabditis elegans RIM (also known as unc-10) may be involved in the regulation of defecation and daumone response. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This RIM-like family domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467198 [Multi-domain]  Cd Length: 95  Bit Score: 37.92  E-value: 4.83e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*...
gi 1958667836   42 IISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDsalEVLRGI-ASETHVVLILR 98
Cdd:cd06714     41 YVTKVKPGSVADTVGHLREGDEVLEWNGISLQGKTFE---EVQDIIsQSKGEVELVVS 95
PDZ_neurabin-like cd06790
PDZ domain of neurabin-1 and neurabin-2, and related domains; PDZ (PSD-95 (Postsynaptic ...
14-95 6.75e-03

PDZ domain of neurabin-1 and neurabin-2, and related domains; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain of neurabin-1 (also known as protein phosphatase 1 regulatory subunit 9A) and neurabin-2 (also known as spinophilin, and protein phosphatase 1 regulatory subunit 9B), and related domains. Neurabin-1 and neurabin-2 are neuronal scaffolding proteins that play important roles in the regulation of synaptic transmission through their ability to interact with and target protein phosphatase 1 (PP1) to dendritic spines where PP1 dephosphorylates and inactivates glutamate receptors. Neurabin-2 interacts with multiple other synaptic proteins, including synaptic signaling and scaffolding proteins (e.g., GluN1 and SAPAP3) and cytoskeletal proteins (e.g., neurofilament medium polypeptide, NF-M). Neurabin-1 and neurabin-2 also binds F-actin. Other binding partners of neurabin-1 include adenosine A1 receptor (A1R), SAD-1 kinase and 70 kDa ribosomal protein S6 kinase (p70-S6K). This PDZ domain is immediately C-terminal to the PP1 binding domain. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This neurabin-like PDZ domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467252 [Multi-domain]  Cd Length: 90  Bit Score: 37.40  E-value: 6.75e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1958667836   14 NVISVRLFKRKVG------GLGFLVKERVSKPPVIISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGI 87
Cdd:cd06790      1 DLFPVELEKGSEGlgisiiGMGVGADAGLEKLGIFVKTVTEGGAAQRDGRIQVNDQIVEVDGISLVGVTQAFAASVLRNT 80

                   ....*...
gi 1958667836   88 ASETHVVL 95
Cdd:cd06790     81 SGTVRFLI 88
PDZ2_ZO1-like_ds cd06728
PDZ domain 2 of Zonula Occludens-1 (ZO-1), ZO-2 and ZO-3, and related domains; form ...
43-98 7.30e-03

PDZ domain 2 of Zonula Occludens-1 (ZO-1), ZO-2 and ZO-3, and related domains; form domain-swapping dimers; PDZ (PSD-95 (Postsynaptic density protein 95), Dlg (Discs large protein), and ZO-1 (Zonula occludens-1)) domain 2 of ZO-1, -2, -3 and related domains. Zonula occludens proteins (ZO-1, ZO-2, ZO-3) are multi-PDZ domain proteins involved in the maintenance and biogenesis of multi-protein networks at the cytoplasmic surface of intercellular contacts in epithelial and endothelial cells. They have three N-terminal PDZ domains, PDZ1-3, followed by a Src homology-3 (SH3) domain and a guanylate kinase (GuK)-like domain. Among protein-protein interactions for all ZO proteins is the binding of the first PDZ domain (PDZ1) to the C-termini of claudins , and the homo- and hetero-dimerization of ZO-proteins via their second PDZ domain (PDZ2), which takes place by symmetrical domain swapping of the first two beta-strands of PDZ2. At the cell level, ZO-1 and ZO-2 are involved in polarity maintenance, gene transcription, cell proliferation, and tumor cell metastasis. PDZ domains usually bind in a sequence-specific manner to short peptide sequences located at the C-terminal end of their partner proteins (known as PDZ binding motifs). The PDZ superfamily includes canonical PDZ domains as well as those with circular permutations and domain swapping mediated by beta-strands. This ZO family PDZ2 domain is a canonical PDZ domain containing six beta-strands A-F and two alpha-helices (alpha-helix 1 and 2), arranged in the order: beta-strands A, B, C, alpha-helix 1, beta-strands D, E, alpha-helix 2 and beta-strand F.


Pssm-ID: 467210 [Multi-domain]  Cd Length: 79  Bit Score: 36.82  E-value: 7.30e-03
                           10        20        30        40        50
                   ....*....|....*....|....*....|....*....|....*....|....*.
gi 1958667836   43 ISDLIRGGAAEQSGLIQAGDIILAVNDRPLVDLSYDSALEVLRGiASETHVVLILR 98
Cdd:cd06728     24 VKEITPDSLAAKDGNLQEGDIILKINGTPVENLSLSEAKKLIEK-SKDKLQLVVLR 78
 
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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