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Role for casein kinase 1 in the phosphorylation of Claspin on critical residues necessary for the activation of Chk1

机译:酪蛋白激酶1在Claspin磷酸化激活Chk1所需的关键残基上的作用

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摘要

The mediator protein Claspin is critical for the activation of the checkpoint kinase Chk1 during checkpoint responses to stalled replication forks. This function involves the Chk1-activating domain (CKAD) of Claspin, which undergoes phosphorylation on multiple conserved sites. These phosphorylations promote binding of Chk1 to Claspin and ensuing activation of Chk1 by ATR. However, despite the importance of this regulatory process, the kinase responsible for these phosphorylations has remained unknown. By using a multifaceted approach, we have found that casein kinase 1 gamma 1 (CK1γ1) carries out this function. CK1γ1 phosphorylates the CKAD of Claspin efficiently in vitro, and depletion of CK1γ1 from human cells by small interfering RNA (siRNA) results in dramatically diminished phosphorylation of Claspin. Consequently, the siRNA-treated cells display impaired activation of Chk1 and resultant checkpoint defects. These results indicate that CK1γ1 is a novel component of checkpoint responses that controls the interaction of a key checkpoint effector kinase with its cognate mediator protein.
机译:介导蛋白Claspin对于检查站对停滞的复制叉的应答过程中检查站激酶Chk1的激活至关重要。此功能涉及Claspin的Chk1激活域(CKAD),该域在多个保守位点进行磷酸化。这些磷酸化促进Chk1与Claspin结合,并随后通过ATR激活Chk1。然而,尽管该调节过程很重要,但负责这些磷酸化的激酶仍是未知的。通过使用多方面的方法,我们发现酪蛋白激酶1γ1(CK1γ1)可以执行此功能。 CK1γ1在体外有效地使Claspin的CKAD磷酸化,而小干扰RNA(siRNA)从人细胞中耗尽CK1γ1导致Claspin的磷酸化大大降低。因此,经siRNA处理的细胞显示出Chk1的激活受损,并导致检查点缺陷。这些结果表明,CK1γ1是检查点反应的新组成部分,它控制关键检查点效应激酶与其同源介体蛋白的相互作用。

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