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Cdk1-Dependent Phosphorylation of Cdc13 Coordinates Telomere Elongation during Cell-Cycle Progression

机译:细胞周期进程中Cdc13依赖性Cdc13磷酸化协调端粒延长

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摘要

Elongation of telomeres by telomerase replenishes the loss of terminal telomeric DNA repeats during each cell cycle. In budding yeast, Cdc13 plays an essential role in telomere length homeostasis, partly through its interactions with both the telomerase complex and the competing Stn1-Ten1 complex. Previous studies in yeast have shown that telomere elongation by telomerase is cell cycle dependent, but the mechanism underlying this dependence is unclear. In S. cerevisiae, a single cyclin-dependent kinase Cdk1 (Cdc28) coordinates the serial events required for the cell division cycle, but no Cdk1 substrate has been identified among telomerase and telomere-associated factors. Here we show that Cdk1-dependent phosphorylation of Cdc13 is essential for efficient recruitment of the yeast telomerase complex to telomeres by favoring the interaction of Cdc13 with Est1 rather than the competing Stn1-Ten1 complex. These results provide a direct mechanistic link between coordination of telomere elongation and cell-cycle progression in vivo.
机译:端粒酶延长端粒延长了每个细胞周期中末端端粒DNA重复序列的丢失。在发芽酵母中,Cdc13在端粒长度稳态中起重要作用,部分原因是它与端粒酶复合物和竞争性Stn1-Ten1复合物的相互作用。以前的酵母研究表明端粒酶延长端粒是细胞周期依赖性的,但这种依赖性的机制尚不清楚。在酿酒酵母中,单个细胞周期蛋白依赖性激酶Cdk1(Cdc28)协调细胞分裂周期所需的系列事件,但端粒酶和端粒相关因子中尚未发现Cdk1底物。在这里,我们显示Cdc13依赖Cdk1的磷酸化通过促进Cdc13与Est1而不是竞争性的Stn1-Ten1复合物的相互作用,对于将酵母端粒酶复合物有效地募集至端粒至关重要。这些结果提供了端粒伸长的协调与体内细胞周期进程之间的直接机械联系。

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