cIAPs Block Ripoptosome Formation, a RIP1/Caspase-8 Containing Intracellular Cell Death Complex Differentially Regulated by cFLIP Isoforms

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• 作者：Maria Feoktistova¹ ; ² ; ⁵ ; Peter Geserick¹ ; ² ; ⁵ ; Beate Kellert¹ ; Diana  ; Panayotova Dimitrova¹ ; Claudia Langlais³ ; Mike Hupe² ; ⁶ ; Kelvin Cain³ ; Marion MacFarlane³ ; Georg Hä ; cker⁴ ; Martin Leverkus¹ ; ² ; ^{martin.leverkus@medma.uni-heidelberg.de"" rel=""nofollow}
• 刊名：Molecular Cell
• 出版年：2011
• 出版时间：5 August 2011
• 年：2011
• 卷：43
• 期：3
• 页码：449-463
• 全文大小：2249 K

文摘

Summary

The intracellular regulation of cell death pathways by cIAPs has been enigmatic. Here we show that loss of cIAPs promotes the spontaneous formation of an intracellular platform that activates either apoptosis or necroptosis. This 2 MDa intracellular complex that we designate “Ripoptosome” is necessary but not sufficient for cell death. It contains RIP1, FADD, caspase-8, caspase-10, and caspase inhibitor cFLIP isoforms. cFLIP_L prevents Ripoptosome formation, whereas, intriguingly, cFLIP_S promotes Ripoptosome assembly. When cIAPs are absent, caspase activity is the “rheostat” that is controlled by cFLIP isoforms in the Ripoptosome and decides if cell death occurs by RIP3-dependent necroptosis or caspase-dependent apoptosis. RIP1 is the core component of the complex. As exemplified by our studies for TLR3 activation, our data argue that the Ripoptosome critically influences the outcome of membrane-bound receptor triggering. The differential quality of cell death mediated by the Ripoptosome may cause important pathophysiological consequences during inflammatory responses.