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首页> 外文期刊>Cell death and differentiation >The role of CAP3 in CD95 signaling: new insights into the mechanism of procaspase-8 activation.
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The role of CAP3 in CD95 signaling: new insights into the mechanism of procaspase-8 activation.

机译:CAP3在CD95信号传导中的作用:对procaspase-8激活机制的新见解。

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摘要

Formation of the CD95 (APO-1/Fas) death inducing signaling complex (DISC) plays a central role in CD95 signaling. Previously, CD95 DISC composition was analyzed by two-dimensional gel electrophoresis and four major cytotoxicity-associated proteins (CAP1-4) were found. CAP1 and CAP2 were defined to be unmodified and phosphorylated FADD, respectively. CAP4 was identified as procaspase-8a. CAP3, however, has remained elusive. In this study, we demonstrate that CAP3 is an intermediate of procaspase-8 processing. CAP3 is generated within seconds of DISC formation and subsequently processed to the prodomain of procaspase-8a that is known as p26 (CAP5). These findings lead to new insights into the mechanism of procaspase-8 processing and apoptosis initiation.
机译:CD95(APO-1 / Fas)死亡诱导信号复合物(DISC)的形成在CD95信号中起着核心作用。以前,通过二维凝胶电泳分析CD95 DISC的组成,发现了四个主要的细胞毒性相关蛋白(CAP1-4)。 CAP1和CAP2分别定义为未修饰和磷酸化的FADD。 CAP4被鉴定为procaspase-8a。但是,CAP3仍然难以捉摸。在这项研究中,我们证明CAP3是procaspase-8加工的中间体。 CAP3在DISC形成的几秒钟内生成,然后被处理为procaspase-8a的前结构域,即p26(CAP5)。这些发现导致对procaspase-8加工和凋亡启动机制的新见解。

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