48887BiochemicalReaction1178

Source:http://www.reactome.org/biopax/48887BiochemicalReaction1178

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Predicate	Object
rdf:type	biopax3:BiochemicalReaction
biopax3:comment	Authored: Garapati, P V, 2009-02-24 10:31:15, Edited: Garapati, P V, 2009-02-24 10:58:20, Phosphorylation of Tyr397 in FAK triggers the phosphorylation of other tyrosine residues (Tyr407, Tyr576, Tyr577, Tyr861 and Tyr925) in a Src-dependent manner. The initial phosphorylation of FAK at Tyr397 is thought to create a high-affinity binding site for SH2 domains, enabling formation of a signalling complex between FAK and members of the Src-family kinases. Tyr-576 and Tyr-577 are located in the central catalytic domain and their phosphorylation is required for the maximum kinase activity of FAK. The tyrosine phosphorylation of these residues is likely to be mediated by Src (or other members of the src family)., Reviewed: Maness, PF, Walmod, PS, 2009--0-5-
biopax3:xref	http://identifiers.org/pubmed/12387730, http://identifiers.org/pubmed/7529876, urn:biopax:UnificationXref:REACTOME DATABASE ID_391866, urn:biopax:UnificationXref:REACTOME_REACT_18385_2
biopax3:dataSource	http://www.reactome.org/biopax/48887Provenance1, urn:biopax:Provenance:reactome_hm_41
biopax3:displayName	Phosphorylation of FAK by Src kinase
biopax3:eCNumber	2.7.10
biopax3:left	http://www.reactome.org/biopax/48887Complex1436, http://www.reactome.org/biopax/48887SmallMolecule1
biopax3:participantStoichio...	http://www.reactome.org/biopax/48887Stoichiometry4148, http://www.reactome.org/biopax/48887Stoichiometry4151
biopax3:right	http://www.reactome.org/biopax/48887SmallMolecule2, http://www.reactome.org/biopax/48887Complex1437