Human Interaction Network Ontology - RIP3 binds TRIF to mediate necroptosis - Classes | NCBO BioPortal

Human Interaction Network Ontology

Last uploaded: June 27, 2014

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Preferred Name	RIP3 binds TRIF to mediate necroptosis
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Definitions	Reviewed: Fitzgerald, Katherine A, 2012-11-13 has a Stoichiometric coefficient of 4 Authored: Shamovsky, V, 2012-05-15 TLR3 and TLR4 -directed programmed necrosis (necroptosis) is mediated by the TRIF-RIP3 pathway in mouse macrophages [He S e al 2011]. RIP3 was shown to be essential mediator in TLR3-induced necroptotic cell death in human epithelial cell lines. Knockdown of RIP3 in human keratinocyte HaCaT cells blocked TLR3-mediated necroptosis without affecting the apoptotic response. Moreover, overexpression of RIP3 in human epithelial carcinoma cell line HeLa led to increased caspase-independent TLR3-induced cell death in the absence of IAPs [Feoktistova M et al 2011]. In addition, in caspase-8- or FADD-deficient human Jurkat cells dsRNA induced programmed necrosis, instead of apoptosis [Kalai M et al 2002]. Thus, when caspase-dependent apoptosis is inhibited or absent, the alternative RIP3-mediated programmed cell death is induced. Edited: Shamovsky, V, 2012-11-19
ID	http://purl.obolibrary.org/obo/HINO_0009313
comment	Reviewed: Fitzgerald, Katherine A, 2012-11-13 has a Stoichiometric coefficient of 4 Authored: Shamovsky, V, 2012-05-15 TLR3 and TLR4 -directed programmed necrosis (necroptosis) is mediated by the TRIF-RIP3 pathway in mouse macrophages [He S e al 2011]. RIP3 was shown to be essential mediator in TLR3-induced necroptotic cell death in human epithelial cell lines. Knockdown of RIP3 in human keratinocyte HaCaT cells blocked TLR3-mediated necroptosis without affecting the apoptotic response. Moreover, overexpression of RIP3 in human epithelial carcinoma cell line HeLa led to increased caspase-independent TLR3-induced cell death in the absence of IAPs [Feoktistova M et al 2011]. In addition, in caspase-8- or FADD-deficient human Jurkat cells dsRNA induced programmed necrosis, instead of apoptosis [Kalai M et al 2002]. Thus, when caspase-dependent apoptosis is inhibited or absent, the alternative RIP3-mediated programmed cell death is induced. Edited: Shamovsky, V, 2012-11-19
definition source	Pubmed12181749 Pubmed22123964 Reactome, http://www.reactome.org Pubmed15814722 Pubmed21737330
has input	http://purl.obolibrary.org/obo/UniProt_Q9Y572 http://purl.obolibrary.org/obo/HINO_0005701
has output	http://purl.obolibrary.org/obo/HINO_0005774
label	RIP3 binds TRIF to mediate necroptosis
prefixIRI	HINO:0009313
prefLabel	RIP3 binds TRIF to mediate necroptosis
seeAlso	ReactomeREACT_150365 GENE ONTOLOGYGO:0060555 Reactome Database ID Release 432569057
subClassOf	http://purl.obolibrary.org/obo/INO_0000040

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