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Conserved domains on  [gi|1143077020|ref|NP_001335203|]
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protein Dok-7 isoform 2 [Mus musculus]

Protein Classification

docking protein 7( domain architecture ID 10199825)

docking protein 7 is a probable muscle-intrinsic activator of MuSK (Muscle-Specific Protein Tyrosine Kinase) that plays an essential role in neuromuscular synaptogenesis

Gene Symbol:  DOK7
Gene Ontology:  GO:0019901|GO:0061098|GO:0007528|GO:0008289
PubMed:  15567406|8987385|10610414|15493994|22728242

Graphical summary

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List of domain hits

 Name Accession Description Interval E-value
PH_DOK7 cd14677
Pleckstrin homology (PH) domain of Downstream of tyrosine kinase 7; The Dok family adapters ...
 6-107 3.66e-62

Pleckstrin homology (PH) domain of Downstream of tyrosine kinase 7; The Dok family adapters are phosphorylated by different protein tyrosine kinases. Dok proteins are involved in processes such as modulation of cell differentiation and proliferation, as well as in control of the cell spreading and migration The Dok protein contains an N-terminal pleckstrin homology (PH) domain followed by a central phosphotyrosine binding (PTB) domain, which has a PH-like fold, and a proline- and tyrosine-rich C-terminal tail. The PH domain is binds to acidic phospholids and localizes proteins to the plasma membrane. There are 7 mammalian Dok members: Dok-1 to Dok-7. Dok-7 is the key cytoplasmic activator of MuSK (Muscle-Specific Protein Tyrosine Kinase). In general, PH domains have diverse functions, but are generally involved in targeting proteins to the appropriate cellular location or in the interaction with a binding partner. They share little sequence conservation, but all have a common fold, which is electrostatically polarized. PH domains are found in cellular signaling proteins such as serine/threonine kinase, tyrosine kinases, regulators of G-proteins, endocytotic GTPases, adaptors, as well as cytoskeletal associated molecules and in lipid associated enzymes.


:

Pssm-ID: 270196  Cd Length: 102  Bit Score: 198.09  E-value: 3.66e-62
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020   6 LVEGQVKLRDGKKWKSRWLVLRKPSPVADCLLMLVYKDKCERSKGLRERSSLTLEDICGLEPALPYEGLAHTLAIICLSQ 85
Cdd:cd14677     1 LVEGQVKLRDGKKWKSRWLVLRKPSPVADCLLLLVYKDKSSRRKGLKEKASLTLEHFCGLESGFPLEKESNTLAIICLTQ 80

                          90       100
                  ....*....|....*....|..
gi 1143077020  86 AVMLGFDSHEAMCAWDTRIRYA 107
Cdd:cd14677    81 VVVLGFDSREALLEWDARIRYA 102
PTB_DOK7 cd13165
Downstream of tyrosine kinase 7 phosphotyrosine-binding domain (PTBi); The Dok family adapters ...
 108-208 1.09e-58

Downstream of tyrosine kinase 7 phosphotyrosine-binding domain (PTBi); The Dok family adapters are phosphorylated by different protein tyrosine kinases. Dok proteins are involved in processes such as modulation of cell differentiation and proliferation, as well as in control of the cell spreading and migration The Dok protein contains an N-terminal pleckstrin homology (PH) domain followed by a central phosphotyrosine binding (PTB) domain, which has a PH-like fold, and a proline- and tyrosine-rich C-terminal tail. The PH domain is binds to acidic phospholids and localizes proteins to the plasma membrane, while the PTB domain mediates protein-protein interactions by binding to phosphotyrosine-containing motifs. The C-terminal part of Dok contains multiple tyrosine phosphorylation sites that serve as potential docking sites for Src homology 2-containing proteins such as ras GTPase-activating protein and Nck, leading to inhibition of ras signaling pathway activation and the c-Jun N-terminal kinase (JNK) and c-Jun activation, respectively. There are 7 mammalian Dok members: Dok-1 to Dok-7. Dok-1 and Dok-2 act as negative regulators of the Ras-Erk pathway downstream of many immunoreceptor-mediated signaling systems, and it is believed that recruitment of p120 rasGAP by Dok-1 and Dok-2 is critical to their negative regulation. Dok-3 is a negative regulator of the activation of JNK and mobilization of Ca2+ in B-cell receptor-mediated signaling, interacting with SHIP-1 and Grb2. Dok-4- 6 play roles in protein tyrosine kinase(PTK)-mediated signaling in neural cells and Dok-7 is the key cytoplasmic activator of MuSK (Muscle-Specific Protein Tyrosine Kinase). PTB domains have a common PH-like fold and are found in various eukaryotic signaling molecules. This domain was initially shown to binds peptides with a NPXY motif with differing requirements for phosphorylation of the tyrosine, although more recent studies have found that some types of PTB domains can bind to peptides lack tyrosine residues altogether. In contrast to SH2 domains, which recognize phosphotyrosine and adjacent carboxy-terminal residues, PTB-domain binding specificity is conferred by residues amino-terminal to the phosphotyrosine. PTB domains are classified into three groups: phosphotyrosine-dependent Shc-like, phosphotyrosine-dependent IRS-like, and phosphotyrosine-independent Dab-like PTB domains. This cd is part of the IRS-like subgroup.


:

Pssm-ID: 269986  Cd Length: 101  Bit Score: 189.26  E-value: 1.09e-58
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020 108 LGEVHRFHVTVAPGTKLESGPATLHLCNDILVLARDIPPTVMGQWKLSDLRRYGAVPNGFIFEGGTRCGYWAGVFFLSSA 187
Cdd:cd13165     1 LGEVHRFPVVVAPGTKLESGPATLHFCNDILVLARDVPPAVLGQWKLSDLRRYGAVPGGFIFEGGTRCGKWAGVFFLSTE 80

                          90       100
                  ....*....|....*....|.
gi 1143077020 188 EGEQMSFLFDCIVRGISPTKG 208
Cdd:cd13165    81 EGEQISFLFDCIVRGISPTKG 101
PHA03307 super family cl33723
transcriptional regulator ICP4; Provisional
 276-487 8.91e-03

transcriptional regulator ICP4; Provisional


The actual alignment was detected with superfamily member PHA03307:

Pssm-ID: 223039 [Multi-domain]  Cd Length: 1352  Bit Score: 39.00  E-value: 8.91e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020  276 SASSRLTAWPEQSSSSAGTSQEGPGLVAAQGPGEAMLGASRPP-LKPLRPRQLQEVGRQSSSDSGIATGSHSSYSGSFSS 354
Cdd:PHA03307   157 ASPAAVASDAASSRQAALPLSSPEETARAPSSPPAEPPPSTPPaAASPRPPRRSSPISASASSPAPAPGRSAADDAGASS 236

                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020  355 YAGSNLDVWRAGEEFGSLLSLPPGASAPEPRlcacPPGAAEYQVPTSLRHhydTPRSLRQAPRDPSPASQGSSDHGSATD 434
Cdd:PHA03307   237 SDSSSSESSGCGWGPENECPLPRPAPITLPT----RIWEASGWNGPSSRP---GPASSSSSPRERSPSPSPSSPGSGPAP 309

                          170       180       190       200       210       220
                   ....*....|....*....|....*....|....*....|....*....|....*....|..
gi 1143077020  435 --------LGGQAPTGCPS-SWLGARRRGQATEGPGSDAALPSPSPGESWEAGSPHAGPPPA 487
Cdd:PHA03307   310 ssprasssSSSSRESSSSStSSSSESSRGAAVSPGPSPSRSPSPSRPPPPADPSSPRKRPRP 371
 
Name Accession Description Interval E-value
PH_DOK7 cd14677
Pleckstrin homology (PH) domain of Downstream of tyrosine kinase 7; The Dok family adapters ...
 6-107 3.66e-62

Pleckstrin homology (PH) domain of Downstream of tyrosine kinase 7; The Dok family adapters are phosphorylated by different protein tyrosine kinases. Dok proteins are involved in processes such as modulation of cell differentiation and proliferation, as well as in control of the cell spreading and migration The Dok protein contains an N-terminal pleckstrin homology (PH) domain followed by a central phosphotyrosine binding (PTB) domain, which has a PH-like fold, and a proline- and tyrosine-rich C-terminal tail. The PH domain is binds to acidic phospholids and localizes proteins to the plasma membrane. There are 7 mammalian Dok members: Dok-1 to Dok-7. Dok-7 is the key cytoplasmic activator of MuSK (Muscle-Specific Protein Tyrosine Kinase). In general, PH domains have diverse functions, but are generally involved in targeting proteins to the appropriate cellular location or in the interaction with a binding partner. They share little sequence conservation, but all have a common fold, which is electrostatically polarized. PH domains are found in cellular signaling proteins such as serine/threonine kinase, tyrosine kinases, regulators of G-proteins, endocytotic GTPases, adaptors, as well as cytoskeletal associated molecules and in lipid associated enzymes.


Pssm-ID: 270196  Cd Length: 102  Bit Score: 198.09  E-value: 3.66e-62
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020   6 LVEGQVKLRDGKKWKSRWLVLRKPSPVADCLLMLVYKDKCERSKGLRERSSLTLEDICGLEPALPYEGLAHTLAIICLSQ 85
Cdd:cd14677     1 LVEGQVKLRDGKKWKSRWLVLRKPSPVADCLLLLVYKDKSSRRKGLKEKASLTLEHFCGLESGFPLEKESNTLAIICLTQ 80

                          90       100
                  ....*....|....*....|..
gi 1143077020  86 AVMLGFDSHEAMCAWDTRIRYA 107
Cdd:cd14677    81 VVVLGFDSREALLEWDARIRYA 102
PTB_DOK7 cd13165
Downstream of tyrosine kinase 7 phosphotyrosine-binding domain (PTBi); The Dok family adapters ...
 108-208 1.09e-58

Downstream of tyrosine kinase 7 phosphotyrosine-binding domain (PTBi); The Dok family adapters are phosphorylated by different protein tyrosine kinases. Dok proteins are involved in processes such as modulation of cell differentiation and proliferation, as well as in control of the cell spreading and migration The Dok protein contains an N-terminal pleckstrin homology (PH) domain followed by a central phosphotyrosine binding (PTB) domain, which has a PH-like fold, and a proline- and tyrosine-rich C-terminal tail. The PH domain is binds to acidic phospholids and localizes proteins to the plasma membrane, while the PTB domain mediates protein-protein interactions by binding to phosphotyrosine-containing motifs. The C-terminal part of Dok contains multiple tyrosine phosphorylation sites that serve as potential docking sites for Src homology 2-containing proteins such as ras GTPase-activating protein and Nck, leading to inhibition of ras signaling pathway activation and the c-Jun N-terminal kinase (JNK) and c-Jun activation, respectively. There are 7 mammalian Dok members: Dok-1 to Dok-7. Dok-1 and Dok-2 act as negative regulators of the Ras-Erk pathway downstream of many immunoreceptor-mediated signaling systems, and it is believed that recruitment of p120 rasGAP by Dok-1 and Dok-2 is critical to their negative regulation. Dok-3 is a negative regulator of the activation of JNK and mobilization of Ca2+ in B-cell receptor-mediated signaling, interacting with SHIP-1 and Grb2. Dok-4- 6 play roles in protein tyrosine kinase(PTK)-mediated signaling in neural cells and Dok-7 is the key cytoplasmic activator of MuSK (Muscle-Specific Protein Tyrosine Kinase). PTB domains have a common PH-like fold and are found in various eukaryotic signaling molecules. This domain was initially shown to binds peptides with a NPXY motif with differing requirements for phosphorylation of the tyrosine, although more recent studies have found that some types of PTB domains can bind to peptides lack tyrosine residues altogether. In contrast to SH2 domains, which recognize phosphotyrosine and adjacent carboxy-terminal residues, PTB-domain binding specificity is conferred by residues amino-terminal to the phosphotyrosine. PTB domains are classified into three groups: phosphotyrosine-dependent Shc-like, phosphotyrosine-dependent IRS-like, and phosphotyrosine-independent Dab-like PTB domains. This cd is part of the IRS-like subgroup.


Pssm-ID: 269986  Cd Length: 101  Bit Score: 189.26  E-value: 1.09e-58
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020 108 LGEVHRFHVTVAPGTKLESGPATLHLCNDILVLARDIPPTVMGQWKLSDLRRYGAVPNGFIFEGGTRCGYWAGVFFLSSA 187
Cdd:cd13165     1 LGEVHRFPVVVAPGTKLESGPATLHFCNDILVLARDVPPAVLGQWKLSDLRRYGAVPGGFIFEGGTRCGKWAGVFFLSTE 80

                          90       100
                  ....*....|....*....|.
gi 1143077020 188 EGEQMSFLFDCIVRGISPTKG 208
Cdd:cd13165    81 EGEQISFLFDCIVRGISPTKG 101
IRS pfam02174
PTB domain (IRS-1 type);
111-192 2.91e-07

PTB domain (IRS-1 type);


Pssm-ID: 460473  Cd Length: 99  Bit Score: 48.40  E-value: 2.91e-07
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020 111 VHRFHVTVAP---GTKLE-SGPATLHLCNDILVLARDIPPTVMGQWKLSDLRRYGAVPNGFIFEGGTRCGYWAGVFFLSS 186
Cdd:pfam02174   1 VEVFPVTVRRtgaSERCGlSGSYRLCLTAEALTLDKLNTRVPLVSWPLTSLRRYGRDKNFFSFEAGRRCVTGEGEFWFQT 80


                  ....*.
gi 1143077020 187 AEGEQM 192
Cdd:pfam02174  81 DDAEEI 86
PTBI smart00310
Phosphotyrosine-binding domain (IRS1-like);
117-192 5.25e-04

Phosphotyrosine-binding domain (IRS1-like);


Pssm-ID: 197644  Cd Length: 99  Bit Score: 39.32  E-value: 5.25e-04
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1143077020  117 TVAPGTKLESGPATLHLCNDILVLARDI-PPTVMGQWKLSDLRRYGAVPNGFIFEGGTRCGYWAGVFFLSSAEGEQM 192
Cdd:smart00310  10 TEGLERCPLSGSYRLRLTSEELVLWRGLnPRVELVVWPLLSLRRYGRDKVFFFFEAGRRCVSGPGEFTFQTVVAQEI 86
PHA03307 PHA03307
transcriptional regulator ICP4; Provisional
 276-487 8.91e-03

transcriptional regulator ICP4; Provisional


Pssm-ID: 223039 [Multi-domain]  Cd Length: 1352  Bit Score: 39.00  E-value: 8.91e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020  276 SASSRLTAWPEQSSSSAGTSQEGPGLVAAQGPGEAMLGASRPP-LKPLRPRQLQEVGRQSSSDSGIATGSHSSYSGSFSS 354
Cdd:PHA03307   157 ASPAAVASDAASSRQAALPLSSPEETARAPSSPPAEPPPSTPPaAASPRPPRRSSPISASASSPAPAPGRSAADDAGASS 236

                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020  355 YAGSNLDVWRAGEEFGSLLSLPPGASAPEPRlcacPPGAAEYQVPTSLRHhydTPRSLRQAPRDPSPASQGSSDHGSATD 434
Cdd:PHA03307   237 SDSSSSESSGCGWGPENECPLPRPAPITLPT----RIWEASGWNGPSSRP---GPASSSSSPRERSPSPSPSSPGSGPAP 309

                          170       180       190       200       210       220
                   ....*....|....*....|....*....|....*....|....*....|....*....|..
gi 1143077020  435 --------LGGQAPTGCPS-SWLGARRRGQATEGPGSDAALPSPSPGESWEAGSPHAGPPPA 487
Cdd:PHA03307   310 ssprasssSSSSRESSSSStSSSSESSRGAAVSPGPSPSRSPSPSRPPPPADPSSPRKRPRP 371
 
Name Accession Description Interval E-value
PH_DOK7 cd14677
Pleckstrin homology (PH) domain of Downstream of tyrosine kinase 7; The Dok family adapters ...
 6-107 3.66e-62

Pleckstrin homology (PH) domain of Downstream of tyrosine kinase 7; The Dok family adapters are phosphorylated by different protein tyrosine kinases. Dok proteins are involved in processes such as modulation of cell differentiation and proliferation, as well as in control of the cell spreading and migration The Dok protein contains an N-terminal pleckstrin homology (PH) domain followed by a central phosphotyrosine binding (PTB) domain, which has a PH-like fold, and a proline- and tyrosine-rich C-terminal tail. The PH domain is binds to acidic phospholids and localizes proteins to the plasma membrane. There are 7 mammalian Dok members: Dok-1 to Dok-7. Dok-7 is the key cytoplasmic activator of MuSK (Muscle-Specific Protein Tyrosine Kinase). In general, PH domains have diverse functions, but are generally involved in targeting proteins to the appropriate cellular location or in the interaction with a binding partner. They share little sequence conservation, but all have a common fold, which is electrostatically polarized. PH domains are found in cellular signaling proteins such as serine/threonine kinase, tyrosine kinases, regulators of G-proteins, endocytotic GTPases, adaptors, as well as cytoskeletal associated molecules and in lipid associated enzymes.


Pssm-ID: 270196  Cd Length: 102  Bit Score: 198.09  E-value: 3.66e-62
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020   6 LVEGQVKLRDGKKWKSRWLVLRKPSPVADCLLMLVYKDKCERSKGLRERSSLTLEDICGLEPALPYEGLAHTLAIICLSQ 85
Cdd:cd14677     1 LVEGQVKLRDGKKWKSRWLVLRKPSPVADCLLLLVYKDKSSRRKGLKEKASLTLEHFCGLESGFPLEKESNTLAIICLTQ 80

                          90       100
                  ....*....|....*....|..
gi 1143077020  86 AVMLGFDSHEAMCAWDTRIRYA 107
Cdd:cd14677    81 VVVLGFDSREALLEWDARIRYA 102
PTB_DOK7 cd13165
Downstream of tyrosine kinase 7 phosphotyrosine-binding domain (PTBi); The Dok family adapters ...
 108-208 1.09e-58

Downstream of tyrosine kinase 7 phosphotyrosine-binding domain (PTBi); The Dok family adapters are phosphorylated by different protein tyrosine kinases. Dok proteins are involved in processes such as modulation of cell differentiation and proliferation, as well as in control of the cell spreading and migration The Dok protein contains an N-terminal pleckstrin homology (PH) domain followed by a central phosphotyrosine binding (PTB) domain, which has a PH-like fold, and a proline- and tyrosine-rich C-terminal tail. The PH domain is binds to acidic phospholids and localizes proteins to the plasma membrane, while the PTB domain mediates protein-protein interactions by binding to phosphotyrosine-containing motifs. The C-terminal part of Dok contains multiple tyrosine phosphorylation sites that serve as potential docking sites for Src homology 2-containing proteins such as ras GTPase-activating protein and Nck, leading to inhibition of ras signaling pathway activation and the c-Jun N-terminal kinase (JNK) and c-Jun activation, respectively. There are 7 mammalian Dok members: Dok-1 to Dok-7. Dok-1 and Dok-2 act as negative regulators of the Ras-Erk pathway downstream of many immunoreceptor-mediated signaling systems, and it is believed that recruitment of p120 rasGAP by Dok-1 and Dok-2 is critical to their negative regulation. Dok-3 is a negative regulator of the activation of JNK and mobilization of Ca2+ in B-cell receptor-mediated signaling, interacting with SHIP-1 and Grb2. Dok-4- 6 play roles in protein tyrosine kinase(PTK)-mediated signaling in neural cells and Dok-7 is the key cytoplasmic activator of MuSK (Muscle-Specific Protein Tyrosine Kinase). PTB domains have a common PH-like fold and are found in various eukaryotic signaling molecules. This domain was initially shown to binds peptides with a NPXY motif with differing requirements for phosphorylation of the tyrosine, although more recent studies have found that some types of PTB domains can bind to peptides lack tyrosine residues altogether. In contrast to SH2 domains, which recognize phosphotyrosine and adjacent carboxy-terminal residues, PTB-domain binding specificity is conferred by residues amino-terminal to the phosphotyrosine. PTB domains are classified into three groups: phosphotyrosine-dependent Shc-like, phosphotyrosine-dependent IRS-like, and phosphotyrosine-independent Dab-like PTB domains. This cd is part of the IRS-like subgroup.


Pssm-ID: 269986  Cd Length: 101  Bit Score: 189.26  E-value: 1.09e-58
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020 108 LGEVHRFHVTVAPGTKLESGPATLHLCNDILVLARDIPPTVMGQWKLSDLRRYGAVPNGFIFEGGTRCGYWAGVFFLSSA 187
Cdd:cd13165     1 LGEVHRFPVVVAPGTKLESGPATLHFCNDILVLARDVPPAVLGQWKLSDLRRYGAVPGGFIFEGGTRCGKWAGVFFLSTE 80

                          90       100
                  ....*....|....*....|.
gi 1143077020 188 EGEQMSFLFDCIVRGISPTKG 208
Cdd:cd13165    81 EGEQISFLFDCIVRGISPTKG 101
PTB_DOK4_DOK5_DOK6 cd13164
Downstream of tyrosine kinase 4, 5, and 6 proteins phosphotyrosine-binding domain (PTBi); The ...
 113-192 1.60e-08

Downstream of tyrosine kinase 4, 5, and 6 proteins phosphotyrosine-binding domain (PTBi); The Dok family adapters are phosphorylated by different protein tyrosine kinases. Dok proteins are involved in processes such as modulation of cell differentiation and proliferation, as well as in control of the cell spreading and migration The Dok protein contains an N-terminal pleckstrin homology (PH) domain followed by a central phosphotyrosine binding (PTB) domain, which has a PH-like fold, and a proline- and tyrosine-rich C-terminal tail. The PH domain binds to acidic phospholids and localizes proteins to the plasma membrane, while the PTB domain mediates protein-protein interactions by binding to phosphotyrosine-containing motifs. The C-terminal part of Dok contains multiple tyrosine phosphorylation sites that serve as potential docking sites for Src homology 2-containing proteins such as ras GTPase-activating protein and Nck, leading to inhibition of ras signaling pathway activation and the c-Jun N-terminal kinase (JNK) and c-Jun activation, respectively. There are 7 mammalian Dok members: Dok-1 to Dok-7. Dok-1 and Dok-2 act as negative regulators of the Ras-Erk pathway downstream of many immunoreceptor-mediated signaling systems, and it is believed that recruitment of p120 rasGAP by Dok-1 and Dok-2 is critical to their negative regulation. Dok-3 is a negative regulator of the activation of JNK and mobilization of Ca2+ in B-cell receptor-mediated signaling, interacting with SHIP-1 and Grb2. Dok-4- 6 play roles in protein tyrosine kinase(PTK)-mediated signaling in neural cells and Dok-7 is the key cytoplasmic activator of MuSK (Muscle-Specific Protein Tyrosine Kinase). PTB domains have a common PH-like fold and are found in various eukaryotic signaling molecules. This domain was initially shown to binds peptides with a NPXY motif with differing requirements for phosphorylation of the tyrosine, although more recent studies have found that some types of PTB domains can bind to peptides lack tyrosine residues altogether. In contrast to SH2 domains, which recognize phosphotyrosine and adjacent carboxy-terminal residues, PTB-domain binding specificity is conferred by residues amino-terminal to the phosphotyrosine. PTB domains are classified into three groups: phosphotyrosine-dependent Shc-like, phosphotyrosine-dependent IRS-like, and phosphotyrosine-independent Dab-like PTB domains. This cd is part of the IRS-like subgroup.


Pssm-ID: 241318  Cd Length: 103  Bit Score: 52.43  E-value: 1.60e-08
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020 113 RFHVTVAPGTKLE-SGPATLHLCNDILVLArDI--PPTVMGQWKLSDLRRYGAVPNGFIFEGGTRCGYWAGVFFLSSAEG 189
Cdd:cd13164     6 RFNVFLLPSPNLDvYGECLLQITHENIYLW-DIhnPRVKLVSWPLCSLRRYGRDSTWFTFEAGRMCDTGEGLFTFQTREG 84


                  ...
gi 1143077020 190 EQM 192
Cdd:cd13164    85 EQI 87
IRS pfam02174
PTB domain (IRS-1 type);
111-192 2.91e-07

PTB domain (IRS-1 type);


Pssm-ID: 460473  Cd Length: 99  Bit Score: 48.40  E-value: 2.91e-07
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020 111 VHRFHVTVAP---GTKLE-SGPATLHLCNDILVLARDIPPTVMGQWKLSDLRRYGAVPNGFIFEGGTRCGYWAGVFFLSS 186
Cdd:pfam02174   1 VEVFPVTVRRtgaSERCGlSGSYRLCLTAEALTLDKLNTRVPLVSWPLTSLRRYGRDKNFFSFEAGRRCVTGEGEFWFQT 80


                  ....*.
gi 1143077020 187 AEGEQM 192
Cdd:pfam02174  81 DDAEEI 86
PTB_FRS2 cd01202
Fibroblast growth factor receptor substrate 2 phosphotyrosine-binding domain; FRS2 (also ...
 109-196 4.40e-07

Fibroblast growth factor receptor substrate 2 phosphotyrosine-binding domain; FRS2 (also called Suc1-associated neurotrophic factor (SNT)-induced tyrosine-phosphorylated target) proteins are membrane-anchored adaptor proteins. They are composed of an N-terminal myristoylation site followed by a phosphotyrosine binding (PTB) domain, which has a PH-like fold, and a C-terminal effector domain containing multiple tyrosine and serine/threonine phosphorylation site. The FRS2/SNT proteins show increased tyrosine phosphorylation by activated receptors, such as fibroblast growth factor receptor (FGFR) and TrkA, recruit SH2 domain containing proteins such as Grb2, and mediate signals from activated receptors to a variety of downstream pathways. The PTB domains of the SNT proteins directly interact with the canonical NPXpY motif of TrkA in a phosphorylationdependent manner, they directly bind to the juxtamembrane region of FGFR in a phosphorylation-independent manner. PTB domains have a common PH-like fold and are found in various eukaryotic signaling molecules. This domain was initially shown to binds peptides with a NPXY motif with differing requirements for phosphorylation of the tyrosine, although more recent studies have found that some types of PTB domains can bind to peptides lack tyrosine residues altogether. In contrast to SH2 domains, which recognize phosphotyrosine and adjacent carboxy-terminal residues, PTB-domain binding specificity is conferred by residues amino-terminal to the phosphotyrosine. PTB domains are classified into three groups: phosphotyrosine-dependent Shc-like, phosphotyrosine-dependent IRS-like, and phosphotyrosine-independent Dab-like PTB domains. This cd is part of the IRS-like subgroup.


Pssm-ID: 269913  Cd Length: 92  Bit Score: 47.96  E-value: 4.40e-07
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020 109 GEVHRFHVTVAPGTKLESGPATLHLCNDILVL-ARDIPPTVmgqWKLSDLRRYGAVPNGFIFEGGTRCGYWAGVFFLSSA 187
Cdd:cd01202     2 LHPNIFKVINVDDDGNELGSGILEVTETELILyQRGKEPVR---WPLLCLRRYGYDSNLFSFESGRRCATGEGIYAFKCK 78


                  ....*....
gi 1143077020 188 EGEQMSFLF 196
Cdd:cd01202    79 RAEELFNLV 87
PH cd00821
Pleckstrin homology (PH) domain; PH domains have diverse functions, but in general are ...
 8-100 5.12e-06

Pleckstrin homology (PH) domain; PH domains have diverse functions, but in general are involved in targeting proteins to the appropriate cellular location or in the interaction with a binding partner. They share little sequence conservation, but all have a common fold, which is electrostatically polarized. Less than 10% of PH domains bind phosphoinositide phosphates (PIPs) with high affinity and specificity. PH domains are distinguished from other PIP-binding domains by their specific high-affinity binding to PIPs with two vicinal phosphate groups: PtdIns(3,4)P2, PtdIns(4,5)P2 or PtdIns(3,4,5)P3 which results in targeting some PH domain proteins to the plasma membrane. A few display strong specificity in lipid binding. Any specificity is usually determined by loop regions or insertions in the N-terminus of the domain, which are not conserved across all PH domains. PH domains are found in cellular signaling proteins such as serine/threonine kinase, tyrosine kinases, regulators of G-proteins, endocytotic GTPases, adaptors, as well as cytoskeletal associated molecules and in lipid associated enzymes.


Pssm-ID: 275388 [Multi-domain]  Cd Length: 92  Bit Score: 44.84  E-value: 5.12e-06
                          10        20        30        40        50        60        70        80
                  ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020   8 EGQVKLRDG---KKWKSRWLVLRKpspvaDCLlmLVYKDKCERSKGLRErsSLTLEDICGLEPALPYEGlAHTLAIICLS 84
Cdd:cd00821     2 EGYLLKRGGgglKSWKKRWFVLFE-----GVL--LYYKSKKDSSYKPKG--SIPLSGILEVEEVSPKER-PHCFELVTPD 71

                          90
                  ....*....|....*..
gi 1143077020  85 QAVM-LGFDSHEAMCAW 100
Cdd:cd00821    72 GRTYyLQADSEEERQEW 88
PTBI smart00310
Phosphotyrosine-binding domain (IRS1-like);
117-192 5.25e-04

Phosphotyrosine-binding domain (IRS1-like);


Pssm-ID: 197644  Cd Length: 99  Bit Score: 39.32  E-value: 5.25e-04
                           10        20        30        40        50        60        70
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*..
gi 1143077020  117 TVAPGTKLESGPATLHLCNDILVLARDI-PPTVMGQWKLSDLRRYGAVPNGFIFEGGTRCGYWAGVFFLSSAEGEQM 192
Cdd:smart00310  10 TEGLERCPLSGSYRLRLTSEELVLWRGLnPRVELVVWPLLSLRRYGRDKVFFFFEAGRRCVSGPGEFTFQTVVAQEI 86
PHA03307 PHA03307
transcriptional regulator ICP4; Provisional
 276-487 8.91e-03

transcriptional regulator ICP4; Provisional


Pssm-ID: 223039 [Multi-domain]  Cd Length: 1352  Bit Score: 39.00  E-value: 8.91e-03
                           10        20        30        40        50        60        70        80
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020  276 SASSRLTAWPEQSSSSAGTSQEGPGLVAAQGPGEAMLGASRPP-LKPLRPRQLQEVGRQSSSDSGIATGSHSSYSGSFSS 354
Cdd:PHA03307   157 ASPAAVASDAASSRQAALPLSSPEETARAPSSPPAEPPPSTPPaAASPRPPRRSSPISASASSPAPAPGRSAADDAGASS 236

                           90       100       110       120       130       140       150       160
                   ....*....|....*....|....*....|....*....|....*....|....*....|....*....|....*....|
gi 1143077020  355 YAGSNLDVWRAGEEFGSLLSLPPGASAPEPRlcacPPGAAEYQVPTSLRHhydTPRSLRQAPRDPSPASQGSSDHGSATD 434
Cdd:PHA03307   237 SDSSSSESSGCGWGPENECPLPRPAPITLPT----RIWEASGWNGPSSRP---GPASSSSSPRERSPSPSPSSPGSGPAP 309

                          170       180       190       200       210       220
                   ....*....|....*....|....*....|....*....|....*....|....*....|..
gi 1143077020  435 --------LGGQAPTGCPS-SWLGARRRGQATEGPGSDAALPSPSPGESWEAGSPHAGPPPA 487
Cdd:PHA03307   310 ssprasssSSSSRESSSSStSSSSESSRGAAVSPGPSPSRSPSPSRPPPPADPSSPRKRPRP 371
 
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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