Ablation of the Raf-1 protein causes fetal liver apoptosis, embryonic lethality, and selective hypersensitivity to Fas-induced cell death. Furthermore, Raf-1–deficient cells show defective migration as a result of the deregulation of the Rho effector kinase Rok-α. In this study, we show that the kinase-independent modulation of Rok-α signaling is also the basis of the antiapoptotic function of Raf-1. Fas activation stimulates the formation of Raf-1–Rok-α complexes, and Rok-α signaling is up-regulated in Raf-1–deficient cells. This leads to increased clustering and membrane expression of Fas, which is rescued both by kinase-dead Raf-1 and by interfering with Rok-α or its substrate ezrin. Increased Fas clustering and membrane expression are also evident in the livers of Raf-1–deficient embryos, and genetically reducing Fas expression counteracts fetal liver apoptosis, embryonic lethality, and the apoptotic defects of embryonic fibroblasts. Thus, Raf-1 has an essential function in regulating Fas expression and setting the threshold of Fas sensitivity during embryonic life.
Raf-1 sets the threshold of Fas sensitivity by modulating Rok-α signaling
D. Piazzolla and K. Meissl contributed equally to this work.
Abbreviations used in this paper: DISC, death-inducing signaling complex; DN, dominant negative; ERK, extracellular regulated kinase; ERM, ezrin–radixin–moesin; FADD, Fas-associating death domain–containing protein; FLIP, FADD-like ice–like inhibitory protein; IP, immunoprecipitate; KC, kinase competent; KD, kinase dead; KO, knockout; MEF, mouse embryonic fibroblast; MEK, mitogen and ERK kinase; PEF, primary MEF; SCR, scrambled; siRNA, small interfering RNA; TNFR, TNF receptor; WT, wild type.
Daniela Piazzolla, Katrin Meissl, Lucia Kucerova, Cristina Rubiolo, Manuela Baccarini; Raf-1 sets the threshold of Fas sensitivity by modulating Rok-α signaling . J Cell Biol 19 December 2005; 171 (6): 1013–1022. doi: https://doi.org/10.1083/jcb.200504137
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