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首页> 外文期刊>Journal of Cell Science >Cyclin E-dependent localization of MCM5 regulates centrosome duplication.
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Cyclin E-dependent localization of MCM5 regulates centrosome duplication.

机译:依赖细胞周期蛋白E的MCM5定位调节中心体复制。

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摘要

Centrosomes are the primary microtubule-organizing centers in animal cells and are required for bipolar spindle assembly during mitosis. Amplification of centrosome number is commonly observed in human cancer cells and might contribute to genomic instability. Cyclin E-Cdk2 has been implicated in regulating centrosome duplication both in Xenopus embryos and extracts and in mammalian cells. Localization of cyclin E on centrosomes is mediated by a 20-amino acid domain termed the centrosomal localization sequence (CLS). In this paper, cyclin E is shown to directly interact with and colocalize on centrosomes with the DNA replication factor MCM5 in a CLS-dependent but Cdk2-independent manner. The domain in MCM5 that is responsible for interaction with cyclin E is distinct from any previously described for MCM5 function and is highly conserved in MCM5 proteins from yeast to mammals. Expression of MCM5 or its cyclin E-interacting domain, but not MCM2, significantly inhibits over-duplication of centrosomes in CHO cells arrested in S-phase. These results indicate that proteins involved in DNA replication might also regulate centrosome duplication.
机译:中心体是动物细胞中主要的微管组织中心,是有丝分裂期间双极纺锤体组装所必需的。在人类癌细胞中通常观察到中心体数目的扩增,并且可能导致基因组不稳定。 Cyclin E-Cdk2与非洲爪蟾胚胎和提取物中以及哺乳动物细胞中的中心体复制有牵连。细胞周期蛋白E在中心体上的定位是由20个氨基酸的结构域介导的,称为中心体定位序列(CLS)。在本文中,显示出细胞周期蛋白E以CLS依赖性但Cdk2依赖性的方式直接与具有DNA复制因子MCM5的中心体相互作用并共定位。 MCM5中负责与细胞周期蛋白E相互作用的结构域与先前描述的MCM5功能不同,并且在从酵母到哺乳动物的MCM5蛋白中高度保守。 MCM5或其细胞周期蛋白E相互作用域的表达,而不是MCM2的表达,显着抑制在S期停滞的CHO细胞中中心体的过度复制。这些结果表明,参与DNA复制的蛋白质也可能调节中心体复制。

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