Human Interaction Network Ontology - IRAK1 or IRAK2 binds to the activated IRAK4 :activated TLR:MyD88:Mal complex - Classes | NCBO BioPortal

Human Interaction Network Ontology

Last uploaded: June 27, 2014

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Preferred Name	IRAK1 or IRAK2 binds to the activated IRAK4 :activated TLR:MyD88:Mal complex
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Definitions	Authored: de Bono, B, 2005-08-16 10:54:15 Reviewed: Gay, NJ, 2006-04-24 16:48:17 has a Stoichiometric coefficient of 4 Reviewed: Napetschnig, Johanna, 2012-11-16 Edited: Shamovsky, V, 2012-11-06 IRAK1 is recruited to the TLR complex through binding with IRAK4[Lin SC et al 2010].<p> Reviewed: Gillespie, ME, 2010-11-30 IRAK2 has been implicated in IL1R and TLR signaling by the observation that IRAK2 can associate with MyD88 and Mal (Muzio et al. 1997). Like IRAK1, IRAK2 is activated downstream of IRAK4 (Kawagoe et al. 2008). It has been suggested that IRAK1 activates IRAK2 (Wesche et al. 1999) but IRAK2 phosphorylation is observed in IRAK1â/â mouse macrophages while IRAK4 deficiency abrogates IRAK2 phosphorylation (Kawagoe et al. 2008), suggesting that activated IRAK4 phosphorylates IRAK2 as it does IRAK1. IL6 production in response to IL1beta is impaired in embryonic fibroblasts from IRAK1 or IRAK2 knockout mice and abrogated in IRAK1/2 dual knockouts (Kawagoe et al. 2007) suggesting that IRAK1 and IRAK2 are both involved in IL1R signaling downstream of IRAK4.
ID	http://purl.obolibrary.org/obo/HINO_0009150
comment	Authored: de Bono, B, 2005-08-16 10:54:15 Reviewed: Gay, NJ, 2006-04-24 16:48:17 has a Stoichiometric coefficient of 4 Reviewed: Napetschnig, Johanna, 2012-11-16 Edited: Shamovsky, V, 2012-11-06 IRAK1 is recruited to the TLR complex through binding with IRAK4[Lin SC et al 2010]. Reviewed: Gillespie, ME, 2010-11-30 IRAK2 has been implicated in IL1R and TLR signaling by the observation that IRAK2 can associate with MyD88 and Mal (Muzio et al. 1997). Like IRAK1, IRAK2 is activated downstream of IRAK4 (Kawagoe et al. 2008). It has been suggested that IRAK1 activates IRAK2 (Wesche et al. 1999) but IRAK2 phosphorylation is observed in IRAK1â/â mouse macrophages while IRAK4 deficiency abrogates IRAK2 phosphorylation (Kawagoe et al. 2008), suggesting that activated IRAK4 phosphorylates IRAK2 as it does IRAK1. IL6 production in response to IL1beta is impaired in embryonic fibroblasts from IRAK1 or IRAK2 knockout mice and abrogated in IRAK1/2 dual knockouts (Kawagoe et al. 2007) suggesting that IRAK1 and IRAK2 are both involved in IL1R signaling downstream of IRAK4.
definition source	Pubmed16024789 Pubmed12150927 Pubmed18438411 Pubmed17890055 Pubmed20485341 Reactome, http://www.reactome.org Pubmed9374458 Pubmed19224918 Pubmed21606490 Pubmed17878161
has input	http://purl.obolibrary.org/obo/HINO_0006043 http://purl.obolibrary.org/obo/HINO_0004306
has output	http://purl.obolibrary.org/obo/HINO_0006045
label	IRAK1 or IRAK2 binds to the activated IRAK4 :activated TLR:MyD88:Mal complex
prefixIRI	HINO:0009150
prefLabel	IRAK1 or IRAK2 binds to the activated IRAK4 :activated TLR:MyD88:Mal complex
seeAlso	Reactome Database ID Release 43166091 ReactomeREACT_6929
subClassOf	http://purl.obolibrary.org/obo/INO_0000040

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