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RPA mediates recombination repair during replication stress and is displaced from DNA by checkpoint signalling in human cells

机译:RPA在复制压力期间介导重组修复,并通过人细胞中的检查点信号传导从DNA置换

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摘要

The replication protein A (RPA) is involved in most, if not all, nuclear metabolism involving single-stranded DNA. Here, we show that RPA is involved in genome maintenance at stalled replication forks by the homologous recombination repair system in humans. Depletion of the RPA protein inhibited the formation of RAD51 nuclear foci after hydroxyurea-induced replication stalling leading to persistent unrepaired DNA double-strand breaks (DSBs). We demonstrate a direct role of RPA in homology directed recombination repair. We find that RPA is dispensable for checkpoint kinase 1 (Chk1) activation and that RPA directly binds RAD52 upon replication stress, suggesting a direct role in recombination repair. In addition we show that inhibition of Chk1 with UCN-01 decreases dissociation of RPA from the chromatin and inhibits association of RAD51 and RAD52 with DNA. Altogether, our data suggest a direct role of RPA in homologous recombination in assembly of the RAD51 and RAD52 proteins. Furthermore, our data suggest that replacement of RPA with the RAD51 and RAD52 proteins is affected by checkpoint signalling. (C) 2007 Elsevier Ltd. All rights reserved.
机译:复制蛋白A(RPA)参与了大多数(如果不是全部)涉及单链DNA的核代谢。在这里,我们显示RPA参与了人类同源重组修复系统在停滞的复制叉处的基因组维护。 RPA蛋白的消耗抑制了羟基脲诱导的复制停滞导致持续的未修复DNA双链断裂(DSB)后,RAD51核病灶的形成。我们证明RPA在同源性定向重组修复中的直接作用。我们发现RPA对于检查点激酶1(Chk1)激活是可有可无的,并且RPA在复制压力下直接结合RAD52,表明在重组修复中具有直接作用。此外,我们表明用UCN-01抑制Chk1会降低RPA从染色质的解离,并抑制RAD51和RAD52与DNA的结合。总而言之,我们的数据表明RPA在RAD51和RAD52蛋白质组装中的同源重组中具有直接作用。此外,我们的数据表明,用RAD51和RAD52蛋白替代RPA会受到检查点信号的影响。 (C)2007 Elsevier Ltd.保留所有权利。

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