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A polycomb group protein, PHF1, is involved in the response to DNA double-strand breaks in human cell

机译:多梳子基团蛋白PHF1参与人类细胞对DNA双链断裂的反应

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摘要

DNA double-strand breaks (DSBs) represent the most toxic DNA damage arisen from endogenous and exogenous genotoxic stresses and are known to be repaired by either homologous recombination or nonhomologous end-joining processes. Although many proteins have been identified to participate in either of the processes, the whole processes still remain elusive. Polycomb group (PcG) proteins are epigenetic chromatin modifiers involved in gene silencing, cancer development and the maintenance of embryonic and adult stem cells. By screening proteins responding to DNA damage using laser micro-irradiation, we found that PHF1, a human homolog of Drosophila polycomb-like, Pcl, protein, was recruited to DSBs immediately after irradiation and dissociated within 10 min. The accumulation at DSBs is Ku70/Ku80-dependent, and knockdown of PHF1 leads to X-ray sensitivity and increases the frequency of homologous recombination in HeLa cell. We found that PHF1 interacts physically with Ku70/Ku80, suggesting that PHF1 promotes nonhomologous end-joining processes. Furthermore, we found that PHF1 interacts with a number of proteins involved in DNA damage responses, RAD50, SMC1, DHX9 and p53, further suggesting that PHF1, besides the function in PcG, is involved in genome maintenance processes.
机译:DNA双链断裂(DSB)代表由内源性和外源性基因毒性胁迫引起的最具毒性的DNA损伤,已知可以通过同源重组或非同源末端连接过程进行修复。尽管已鉴定出许多蛋白质参与其中的任何一个过程,但整个过程仍然难以捉摸。聚梳组(PcG)蛋白是表观遗传染色质修饰剂,参与基因沉默,癌症发展以及胚胎和成体干细胞的维持。通过使用激光微辐射筛选响应DNA损伤的蛋白质,我们发现PHF1(果蝇多梳状,Pcl,蛋白质的人类同源物)在照射后立即募集到DSB中,并在10分钟内解离。 DSB处的积累是Ku70 / Ku80依赖性的,而PHF1的敲低导致X射线敏感性,并增加HeLa细胞中同源重组的频率。我们发现PHF1在物理上与Ku70 / Ku80相互作用,这表明PHF1促进了非同源末端连接过程。此外,我们发现PHF1与许多参与DNA损伤反应的蛋白质相互作用,即RAD50,SMC1,DHX9和p53,这进一步表明PHF1除了PcG中的功能外,还参与基因组维护过程。

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