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Regulation of the cellular DNA double-strand break response.

机译:细胞DNA双链断裂反应的调节。

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DNA double-strand breaks occur frequently in cycling cells, and are also induced by exogenous sources, including ionizing radiation. Cells have developed integrated double-strand break response pathways to cope with these lesions, including pathways that initiate DNA repair (either via homologous recombination or nonhomologous end joining), the cell-cycle checkpoints (G1-S, intra-S phase, and G2-M) that provide time for repair, and apoptosis. However, before any of these pathways can be activated, the damage must first be recognized. In this review, we will discuss how the response of mammalian cells to DNA double-strand breaks is regulated, beginning with the activation of ATM, the pinnacle kinase of the double-strand break signalling cascade.
机译:DNA双链断裂经常在循环细胞中发生,并且也由外源包括电离辐射诱导。细胞已开发出整合的双链断裂应答途径来应对这些病变,包括引发DNA修复的途径(通过同源重组或非同源末端连接),细胞周期检查点(G1-S,S内S期和G2) -M),为修复和凋亡提供时间。但是,在激活任何这些途径之前,必须首先识别损坏。在这篇综述中,我们将讨论如何从DNA双链断裂信号级联的顶峰激酶ATM的活化开始调节哺乳动物细胞对DNA双链断裂的反应。

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