Source:http://www.reactome.org/biopax/48887BiochemicalReaction2818
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Authored: Ray, KP, 2010-05-17,
Edited: Jupe, S, 2010-05-17,
IL1 induces the poly-ubiquitination and degradation of IRAK1. This was believed to be K48-linked polyubiquitination, targeting IRAK1 for proteolysis by the proteasome, but recently IL-1R signaling has been shown to lead to K63-linked polyubiquitination of IRAK1 (Windheim et al. 2008; Conze et al. 2008), and demonstrated to have a role in the activation of NF-kappaB. IRAK1 is ubiquitinated on K134 and K180; mutation of these sites impairs IL1R-mediated ubiquitylation of IRAK1 (Conze et al. 2008). Some authors have proposed a role for TRAF6 as the E3 ubiquitin ligase that catalyzes polyubiquitination of IRAK1 (Conze et al. 2008) but this view has been refuted (Windheim et al. 2008; Xiao et al. 2008). There is stronger agreement that Pellino proteins have a role as IRAK1 E3 ubiquitin ligases. <br>Pellino1-3 possess E3 ligase activity and are believed to directly catalyse polyubiquitylation of IRAK1 (Xiao et al. 2008; Butler et al. 2007; Ordureau et al. 2008). They are capable of catalysing the formation of K63- and K48-linked polyubiquitin chains; the type of linkage is controlled by the collaborating E2 enzyme. All the Pellino proteins can combine with the E2 heterodimer UbcH13â??Uev1a to catalyze K63-linked ubiquitylation (Ordureau et al. 2008).,
Reviewed: Pinteaux, E, 2010-05-17
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| biopax3:xref |
http://identifiers.org/pubmed/16884718,
http://identifiers.org/pubmed/17997719,
http://identifiers.org/pubmed/18180283,
http://identifiers.org/pubmed/18326498,
http://identifiers.org/pubmed/18347055,
http://identifiers.org/pubmed/19022706,
urn:biopax:UnificationXref:REACTOME DATABASE ID_451418,
urn:biopax:UnificationXref:REACTOME_REACT_22381_1
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Pellino ubiquitinates IRAK1
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6.3.2.19
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