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The NEK1 interactor C21ORF2 is required for efficient DNA damage repair

机译:NEK1相互作用子C21ORF2是有效修复DNA损伤所必需的

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摘要

Defective DNA damage response is a threat to genome stability and a proven cause of tumorigenesis. C21ORF2 (chromosome 21 open reading frame 2) is a novel gene on chromosome 21, and the C21ORF2 protein is found to interact with NEK1. Earlier studies showed that C21ORF2 might be associated with some human genetic diseases including Down syndrome. However, the cellular functions of C21ORF2 remain unknown. In the present study, we reported that C21ORF2 affected cell proliferation after DNA damage induced by ionizing radiation, and DNA repair was less efficient in C21ORF2-depleted cells compared with control cells. However, C21ORF2-knockdown cells did not show defects in the activation of the G2-phase DNA damage checkpoint. Furthermore, homologous recombination, but not non-homologous end joining repair, was found to be impaired after C21ORF2 attenuation, which could be rescued by the overexpression of NEK1, indicating that C21ORF2 functions in the same pathway as NEK1 in DNA damage repair.
机译:缺陷的DNA损伤反应是对基因组稳定性的威胁,也是肿瘤发生的可靠原因。 C21ORF2(21号染色体开放阅读框2)是21号染色体上的新基因,并且发现C21ORF2蛋白与NEK1相互作用。早期的研究表明,C21ORF2可能与某些人类遗传疾病有关,包括唐氏综合症。但是,C21ORF2的细胞功能仍然未知。在本研究中,我们报道了C21ORF2在电离辐射诱导的DNA损伤后影响细胞增殖,并且与对照组相比,在C21ORF2耗尽的细胞中DNA修复的效率较低。但是,C21ORF2组合式细胞在G2期DNA损伤检查点的激活中未显示缺陷。此外,发现在C21ORF2减弱后同源重组受损,但在非同源末端连接修复中未受损,这可以通过NEK1的过表达得以挽救,这表明C21ORF2在DNA损伤修复中的作用与NEK1相同。

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