首页> 外文期刊>Philosophical Transactions of the Royal Society of London, Series B. Biological Sciences >Surviving chromosome replication: the many roles of the S-phase checkpoint pathway
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Surviving chromosome replication: the many roles of the S-phase checkpoint pathway

机译:存活的染色体复制:S期检查点途径的许多作用

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摘要

Checkpoints were originally identified as signalling pathways that delay mitosis in response to DNA damage or defects in chromosome replication, allowing time for DNA repair to occur. The ATR (ataxia- and rad-related) and ATM (ataxia-mutated) protein kinases are recruited to defective replication forks or to sites of DNA damage, and are thought to initiate the DNA damage response in all eukaryotes. In addition to delaying cell cycle progression, however, the S-phase checkpoint pathway also controls chromosome replication and DNA repair pathways in a highly complex fashion, in order to preserve genome integrity. Much of our understanding of this regulation has come fromstudies of yeasts, in which the best-characterized targets are the stimulation of ribonucleotide reductase activity by multiple mechanisms, and the inhibition of new initiation events at later origins of DNA replication. In addition, however, the S-phase checkpoint also plays a more enigmatic and apparently critical role in preserving the functional integrity of defective replication forks, by mechanisms that are still understood poorly. This review considers some of the key experiments that have led to our current understanding of this highly complex pathway.
机译:检查点最初被识别为响应DNA损伤或染色体复制缺陷而延迟有丝分裂的信号传导途径,从而有时间进行DNA修复。 ATR(共济失调和rad相关)和ATM(共济失调突变)蛋白激酶被募集到有缺陷的复制叉或DNA损伤位点,并被认为可以引发所有真核生物的DNA损伤反应。但是,除了延迟细胞周期进程外,S期检查点途径还以高度复杂的方式控制染色体复制和DNA修复途径,以保持基因组完整性。我们对这种调节的大部分了解来自酵母的研究,其中最典型的靶标是通过多种机制刺激核糖核苷酸还原酶活性,以及​​在后来的DNA复制起点抑制新的启动事件。但是,此外,S阶段检查点还通过难以理解的机制在维护有缺陷的复制叉的功能完整性方面起着更加神秘的作用,并且显然起着至关重要的作用。这篇评论考虑了一些关键实验,这些实验导致了我们目前对这种高度复杂的途径的理解。

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