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首页> 外文期刊>Molecular cell >Phosphorylation of Mcm2 by Cdc7 promotes pre-replication complex assembly during cell-cycle re-entry.
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Phosphorylation of Mcm2 by Cdc7 promotes pre-replication complex assembly during cell-cycle re-entry.

机译:Cdc7对Mcm2的磷酸化促进了细胞周期再进入过程中复制前复合物的组装。

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摘要

Cyclin E has been shown to have a role in pre-replication complex (Pre-RC) assembly in cells re-entering the cell cycle from quiescence. The assembly of the pre-RC, which involves the loading of six MCM subunits (Mcm2-7), is a prerequisite for DNA replication. We found that cyclin E, through activation of Cdk2, promotes Mcm2 loading onto chromatin. This function is mediated in part by promoting the accumulation of Cdc7 messenger RNA and protein, which then phosphorylates Mcm2. Consistent with this, a phosphomimetic mutant of Mcm2 can bypass the requirement for Cdc7 in terms of Mcm2 loading. Furthermore, ectopic expression of both Cdc6 and Cdc7 can rescue the MCM loading defect associated with expression of dominant-negative Cdk2. These results are consistent with a role for cyclin E-Cdk2 in promoting the accumulation of Cdc6 and Cdc7, which is required for Mcm2 loading when cells re-enter the cell cycle from quiescence.
机译:已经表明,细胞周期蛋白E在细胞中从复制进入重新进入细胞周期的复制前复合体(Pre-RC)组装中起作用。 pre-RC的组装涉及六个MCM亚基(Mcm2-7)的装载,是DNA复制的先决条件。我们发现细胞周期蛋白E通过激活Cdk2促进Mcm2加载到染色质上。该功能部分地通过促进Cdc7信使RNA和蛋白质的积累而介导,然后使Mcm2磷酸化。与此相一致,就Mcm2负载而言,Mcm2的模拟磷酸突变体可以绕过对Cdc7的要求。此外,Cdc6和Cdc7的异位表达可以挽救与显性负Cdk2表达相关的MCM加载缺陷。这些结果与细胞周期蛋白E-Cdk2在促进Cdc6和Cdc7积累中的作用相一致,当细胞从静止状态重新进入细胞周期时,这是Mcm2加载所必需的。

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