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首页> 外文期刊>Cell cycle >Dual functions of DNA replication forks in checkpoint signaling and PCNA ubiquitination.
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Dual functions of DNA replication forks in checkpoint signaling and PCNA ubiquitination.

机译:DNA复制的双重功能在检查点信号和PCNA泛素化中分叉。

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摘要

During cell proliferation, DNA damage inflicted by intrinsic or extrinsic genotoxic stresses impose a threat to DNA replication. The stability of the DNA replication forks that encounter DNA damage is crucial for genomic integrity. Both the ATR-regulated checkpoint pathway and the translesion DNA synthesis mediated by the ubiquitinated PCNA are important for continuous replication of damaged DNA. We have recently shown that Chk1, a key effector kinase of ATR in checkpoint response, is required for efficient PCNA ubiquitination after DNA damage. Surprisingly, the ubiquitination of PCNA is independent of ATR, but regulated by Claspin, a replication protein that mediates the activation of Chk1 by ATR. Like Claspin, Timeless and Rad17, two other Chk1 regulators at stressed replication forks, are also implicated in PCNA ubiquitination. These findings suggest that while ATR signaling and PCNA ubiquitination are two independent processes, they are mediated by a common group of proteins including Chk1 and it regulators at replication forks. Furthermore, these data raise the possibility that Chk1 and its regulators may constitute a functional module at replication forks to enable multiple stress responses.
机译:在细胞增殖过程中,内源性或外源性遗传毒性胁迫造成的DNA损伤对DNA复制构成威胁。遇到DNA损伤的DNA复制叉的稳定性对于基因组完整性至关重要。 ATR调节的检查点途径和泛素化PCNA介导的病灶DNA合成对于受损DNA的连续复制都是重要的。我们最近显示,Chk1,ATR在关卡反应中的关键效应激酶,是DNA损伤后有效PCNA泛素化所必需的。令人惊讶的是,PCNA的泛素化与ATR无关,但由Claspin调控,Claspin是一种介导ATR激活Chk1活化的复制蛋白。像Claspin,Timeless和Rad17一样,PCNA泛素化也与处于压力复制叉的另外两个Chk1调节剂有关。这些发现表明,尽管ATR信号传导和PCNA泛素化是两个独立的过程,但它们是由一组共同的蛋白质介导的,包括Chk1及其在复制叉处的调节子。此外,这些数据还增加了Chk1及其调节剂可能在复制叉处构成功能模块以实现多种压力响应的可能性。

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