首页> 美国卫生研究院文献>Molecular and Cellular Biology >The Phosphatase-Transcription Activator EYA1 Is Targeted by Anaphase-Promoting Complex/Cdh1 for Degradation at M-to-G1 Transition
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The Phosphatase-Transcription Activator EYA1 Is Targeted by Anaphase-Promoting Complex/Cdh1 for Degradation at M-to-G1 Transition

机译:磷酸酶转录激活因子EYA1被后期促进复合物/ Cdh1靶向在M到G1过渡时降解

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摘要

The phosphatase and transactivator EYA family proteins are overexpressed in many cancer cell lines and are abundantly distributed in undifferentiated cells during development. Loss-of-function studies have shown that EYA1 is required for cell proliferation and survival during mammalian organogenesis. However, how EYA1 is regulated during development is unknown. Here, we report that EYA1 is regulated throughout the cell cycle via ubiquitin-mediated proteolysis. The level of EYA1 protein fluctuates in the cell cycle, peaking during mitosis and dropping drastically as cells exit into G1. We found that EYA1 is efficiently degraded during mitotic exit in a Cdh1-dependent manner and that these two proteins physically interact. Overexpression of Cdh1 reduces the protein levels of ectopically expressed or endogenous EYA1, whereas depletion of Cdh1 by RNA interference stabilizes the EYA1 protein. Together, our results indicate that anaphase-promoting complex/cyclosome (APC/C)–Cdh1 specifically targets EYA1 for degradation during M-to-G1 transition, failure of which may compromise cell proliferation and survival.
机译:磷酸酶和反式激活蛋白EYA家族蛋白在许多癌细胞系中过表达,并且在发育过程中大量分布在未分化的细胞中。功能丧失研究表明,EYA1是哺乳动物器官发生过程中细胞增殖和存活所必需的。但是,如何在发育过程中调节EYA1尚不清楚。在这里,我们报告EYA1在整个细胞周期中通过遍在蛋白介导的蛋白水解调节。 EYA1蛋白的水平在细胞周期中波动,在有丝分裂期间达到峰值,并随着细胞进入G1而急剧下降。我们发现,EYA1在有丝分裂退出过程中以Cdh1依赖的方式被有效降解,并且这两种蛋白质在物理上相互作用。 Cdh1的过表达降低了异位表达或内源性EYA1的蛋白水平,而RNA干扰对Cdh1的消耗则稳定了EYA1蛋白。总之,我们的结果表明,后期促进复合物/环体(APC / C)–Cdh1专门针对EYA1在M到G1过渡过程中降解,其失败可能会损害细胞增殖和存活。

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