48887BiochemicalReaction2470

Source:http://www.reactome.org/biopax/48887BiochemicalReaction2470

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Predicate	Object
rdf:type	biopax3:BiochemicalReaction
biopax3:comment	Authored: Shamovsky, V, 2010-08-25, Edited: Shamovsky, V, 2011-08-12, Hyperphosphorylated IRAK1, still within the receptor complex, binds TRAF6 through multiple regions including the death domain, the undefined domain and the C-terminal C1 domain (Li et al. 2001). The C-terminal region of IRAK-1 contains three potential TRAF6-binding sites; mutation of the amino acids (Glu544, Glu587, Glu706) in these sites to alanine greatly reduces activation of NFkappaB (Ye et al. 2002)., IRAK-2 has two TRAF6 binding motifs that are responsible for initiating TRAF6 signaling transduction (Ye H et al 2002). IRAK2 point mutants with mutated TRAF6-binding motifs abrogate NFkB activation and are incapable to stimulate TRAF6 ubiquitination (Keating SE et al 2007)., Reviewed: Gillespie, ME, 2011-02-10, Reviewed: Li, L, 2011-08-04
biopax3:xref	http://identifiers.org/pubmed/11287640, http://identifiers.org/pubmed/12138165, http://identifiers.org/pubmed/12140561, http://identifiers.org/pubmed/17878161, http://identifiers.org/pubmed/18070982, http://identifiers.org/pubmed/8837778, urn:biopax:UnificationXref:REACTOME DATABASE ID_975857, urn:biopax:UnificationXref:REACTOME_REACT_27141_3
biopax3:dataSource	http://www.reactome.org/biopax/48887Provenance1, urn:biopax:Provenance:reactome_hm_41
biopax3:displayName	TRAF6 binds to hp- IRAK1 or p-IRAK2
biopax3:left	http://www.reactome.org/biopax/48887Complex3088, http://www.reactome.org/biopax/48887Protein8212
biopax3:participantStoichio...	http://www.reactome.org/biopax/48887Stoichiometry8593
biopax3:right	http://www.reactome.org/biopax/48887Complex3089