Department of Pharmacology and Cancer Biology, Duke University Medical Center, Durham, NC 27710, USA.
EMBO J. 2012 Mar 7;31(5):1279-92. doi: 10.1038/emboj.2011.491. Epub 2012 Jan 13.
Many pro-apoptotic signals trigger mitochondrial cytochrome c release, leading to caspase activation and ultimate cellular breakdown. Cell survival pathways, including the mitogen-activated protein kinase (MAPK) cascade, promote cell viability by impeding mitochondrial cytochrome c release and by inhibiting subsequent caspase activation. Here, we describe a mechanism for the inhibition of cytochrome c-induced caspase activation by MAPK signalling, identifying a novel mode of apoptotic regulation exerted through Apaf-1 phosphorylation by the 90-kDa ribosomal S6 kinase (Rsk). Recruitment of 14-3-3ɛ to phosphorylated Ser268 impedes the ability of cytochrome c to nucleate apoptosome formation and activate downstream caspases. High endogenous levels of Rsk in PC3 prostate cancer cells or Rsk activation in other cell types promoted 14-3-3ɛ binding to Apaf-1 and rendered the cells insensitive to cytochrome c, suggesting a potential role for Rsk signalling in apoptotic resistance of prostate cancers and other cancers with elevated Rsk activity. Collectively, these results identify a novel locus of apoptosomal regulation wherein MAPK signalling promotes Rsk-catalysed Apaf-1 phosphorylation and consequent binding of 14-3-3ɛ, resulting in decreased cellular responsiveness to cytochrome c.
许多促进细胞凋亡的信号触发线粒体细胞色素 c 的释放,导致半胱天冬酶的激活和最终的细胞破裂。细胞存活途径,包括丝裂原活化蛋白激酶(MAPK)级联反应,通过阻止线粒体细胞色素 c 的释放和抑制随后的半胱天冬酶的激活来促进细胞活力。在这里,我们描述了 MAPK 信号抑制细胞色素 c 诱导的半胱天冬酶激活的机制,确定了一种通过 90kDa 核糖体 S6 激酶(Rsk)对 Apaf-1 的磷酸化来发挥凋亡调节的新方式。磷酸化 Ser268 的 14-3-3ɛ与 Apaf-1 的募集,阻碍了细胞色素 c 引发凋亡小体形成和激活下游半胱天冬酶的能力。PC3 前列腺癌细胞中高内源性 Rsk 水平或其他细胞类型中 Rsk 的激活促进了 14-3-3ɛ与 Apaf-1 的结合,使细胞对细胞色素 c 不敏感,这表明 Rsk 信号在前列腺癌和其他 Rsk 活性升高的癌症中的凋亡抵抗中可能发挥作用。总之,这些结果确定了一个新的凋亡小体调节部位,其中 MAPK 信号促进 Rsk 催化的 Apaf-1 磷酸化和随后的 14-3-3ɛ结合,导致细胞对细胞色素 c 的反应性降低。
