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Coactivator functions in a stoichiometric complex with anaphase-promoting complex/cyclosome to mediate substrate recognition

机译:助活化剂在化学计量配合物中与后期促进配合物/环体一起发挥功能以介导底物识别

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摘要

The anaphase-promoting complex/cyclosome (APC/C) is a multisubunit E3 ligase required for ubiquitin-dependent proteolysis of cell-cycle-regulatory proteins, including mitotic cyclins and securin/Pds1. Regulation of APC/C activity and substrate recognition, mediated by the coactivators Cdc20 and Cdh1, is fundamental to cell-cycle control. However, the precise mechanism by which coactivators stimulate APC/C ubiquitylation activity and the nature of the substrate-binding sites on the activated APC/C are not understood. Here, we show that the optimal interaction of substrate with APC/C is dependent specifically on the simultaneous association of coactivator. This is consistent with a model whereby both core APC/C subunits and coactivators contribute recognition sites for substrates, accounting for the bipartite nature (D and KEN boxes) of most APC/C degradation signals. A direct and stoichiometric function for the coactivators could explain how specific substrates are recognized by APC/C in a cell-cycle-specific manner, and how coactivator stimulates APC/C ubiquitylation activity.
机译:后期促进复合物/环体(APC / C)是细胞周期调节蛋白(包括有丝分裂细胞周期蛋白和securin / Pds1)的泛素依赖性蛋白水解所需的多亚基E3连接酶。由共激活因子Cdc20和Cdh1介导的APC / C活性和底物识别的调控是细胞周期控制的基础。但是,尚不清楚共激活剂刺激APC / C泛素化活性的确切机制以及激活的APC / C上底物结合位点的性质。在这里,我们表明底物与APC / C的最佳相互作用特别取决于共激活剂的同时缔合。这与一个模型一致,在模型中,核心APC / C亚基和共激活剂都为底物贡献了识别位点,这解释了大多数APC / C降解信号的二分性质(D和KEN盒)。共激活剂的直接和化学计量功能可以解释APC / C如何以细胞周期特异性方式识别特定的底物,以及共激活剂如何刺激APC / C的泛素化活性。

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