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Merck

RIP3 induces apoptosis independent of pronecrotic kinase activity.

Molecular cell (2014-12-03)
Pratyusha Mandal, Scott B Berger, Sirika Pillay, Kenta Moriwaki, Chunzi Huang, Hongyan Guo, John D Lich, Joshua Finger, Viera Kasparcova, Bart Votta, Michael Ouellette, Bryan W King, David Wisnoski, Ami S Lakdawala, Michael P DeMartino, Linda N Casillas, Pamela A Haile, Clark A Sehon, Robert W Marquis, Jason Upton, Lisa P Daley-Bauer, Linda Roback, Nancy Ramia, Cole M Dovey, Jan E Carette, Francis Ka-Ming Chan, John Bertin, Peter J Gough, Edward S Mocarski, William J Kaiser
ZUSAMMENFASSUNG

Receptor-interacting protein kinase 3 (RIP3 or RIPK3) has emerged as a central player in necroptosis and a potential target to control inflammatory disease. Here, three selective small-molecule compounds are shown to inhibit RIP3 kinase-dependent necroptosis, although their therapeutic value is undermined by a surprising, concentration-dependent induction of apoptosis. These compounds interact with RIP3 to activate caspase 8 (Casp8) via RHIM-driven recruitment of RIP1 (RIPK1) to assemble a Casp8-FADD-cFLIP complex completely independent of pronecrotic kinase activities and MLKL. RIP3 kinase-dead D161N mutant induces spontaneous apoptosis independent of compound, whereas D161G, D143N, and K51A mutants, like wild-type, only trigger apoptosis when compound is present. Accordingly, RIP3-K51A mutant mice (Rip3(K51A/K51A)) are viable and fertile, in stark contrast to the perinatal lethality of Rip3(D161N/D161N) mice. RIP3 therefore holds both necroptosis and apoptosis in balance through a Ripoptosome-like platform. This work highlights a common mechanism unveiling RHIM-driven apoptosis by therapeutic or genetic perturbation of RIP3.

MATERIALIEN
Produktnummer
Marke
Produktbeschreibung

Sigma-Aldrich
GSK′843, ≥98% (HPLC)