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首页> 外文期刊>Journal of Cell Science >Cep78 is a new centriolar protein involved in Plk4-induced centriole overduplication
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Cep78 is a new centriolar protein involved in Plk4-induced centriole overduplication

机译:Cep78是一种新的着丝粒蛋白,参与Plk4诱导的着丝粒过度复制

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Centrioles are core components of centrosomes, the major microtubule-organizing centers of animal cells, and act as basal bodies for cilia formation. Control of centriole number is therefore crucial for genome stability and embryogenesis. Centriole duplication requires the serine/threonine protein kinase Plk4. Here, we identify Cep78 as a human centrosomal protein and a new interaction partner of Plk4. Cep78 is mainly a centriolar protein that localizes to the centriolar wall. Furthermore, we find that Plk4 binds to Cep78 through its N-terminal domain but that Cep78 is not an in vitro Plk4 substrate. Cep78 colocalizes with Plk4 at centrioles and is required for Plk4-induced centriole overduplication. Interestingly, upon depletion of Cep78, newly synthesized Plk4 is not localized to centrosomes. Our results suggest that the interaction between Cep78 and the N-terminal catalytic domain of Plk4 is a new and important element in the centrosome overduplication process.
机译:着丝粒是着丝粒的核心成分,着丝粒是动物细胞的主要微管组织中心,并充当纤毛形成的基体。因此,对中心粒数的控制对于基因组稳定性和胚胎发生至关重要。重心复制需要丝氨酸/苏氨酸蛋白激酶Plk4。在这里,我们确定Cep78是人类中心体蛋白,是Plk4的新的相互作用伴侣。 Cep78主要是一种定位于中心体壁的中心体蛋白。此外,我们发现Plk4通过其N末端域与Cep78结合,但Cep78不是体外的Plk4底物。 Cep78在中心点与Plk4共定位,并且是Plk4诱导的中心点过度复制所必需的。有趣的是,在Cep78耗尽后,新合成的Plk4并不局限于中心体。我们的结果表明,Cep78与Plk4的N末端催化域之间的相互作用是中心体重复复制过程中的一个新的重要元素。

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