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Dual role for Saccharomyces cerevisiae Tel1 in the checkpoint response to double-strand breaks

机译:酿酒酵母Tel1在检查点对双链断裂反应中的双重作用

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摘要

The main responder to DNA double-strand breaks (DSBs) in mammals is ataxia telangiectasia mutated (ATM), whereas DSB-induced checkpoint activation in budding yeast seems to depend primarily on the ATM and Rad-3-related (ATR) orthologue Mec1. Here, we show that Saccharomyces cerevisiae Tel1, the ATM orthologue, has two functions in checkpoint response to DSBs. First, Tel1 participates, together with the MRX complex, in Mec1-dependent DSB-induced checkpoint activation by increasing the efficiency of single-stranded DNA accumulation at the ends of DSBs, and this checkpoint function can be overcome by overproducing the exonuclease Exo1. Second, Tel1 can activate the checkpoint response to DSBs independently of Mec1, although its signalling activity only becomes apparent when several DSBs are generated. Furthermore, we provide evidence that the kinetics of DSB resection can influence Tel1 activation, indicating that processing of the DSB termini might influence the transition from Tel1/ATM- to Mec1/ATR-dependent checkpoint.
机译:哺乳动物中DNA双链断裂(DSBs)的主要反应是共济失调毛细血管扩张突变(ATM),而DSB诱导的萌芽酵母中的检查点激活似乎主要取决于ATM和Rad-3相关(ATR)直向同源物Mec1。在这里,我们显示啤酒酵母Tel1,ATM直系同源物,在检查站对DSB的响应中具有两个功能。首先,Tel1与MRX复合体一起通过增加DSB末端单链DNA积累的效率来参与Mec1依赖的DSB诱导的检查点激活,并且可以通过过量生产核酸外切酶Exo1来克服此检查点功能。其次,Tel1可以独立于Mec1来激活对DSB的检查点响应,尽管其信令活动仅在生成多个DSB时才变得明显。此外,我们提供了DSB切除动力学可以影响Tel1激活的证据,表明DSB末端的处理可能影响从Tel1 / ATM-到依赖Mec1 / ATR的检查点的过渡。

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