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ATM:基因毒性应激多种反应的介导因子。

ATM: a mediator of multiple responses to genotoxic stress.

作者信息

Rotman G, Shiloh Y

机构信息

Department of Human Genetics and Molecular Medicine, Sackler School of Medicine, Tel Aviv University, Ramat Aviv 69978, Israel.

出版信息

Oncogene. 1999 Nov 1;18(45):6135-44. doi: 10.1038/sj.onc.1203124.

Abstract

The ATM protein kinase is the product of the gene responsible for the pleiotropic recessive disorder ataxia-telangiectasia. ATM-deficient cells show enhanced sensitivity and greatly reduced responses to genotoxic agents that generate DNA double strand breaks (DSBs), such as ionizing radiation and radiomimetic chemicals, but exhibit normal responses to DNA adducts and base modifications induced by other agents. Therefore, DSBs are most likely the predominant signal for the activation of ATM-mediated pathways. Identification of the ATM gene triggered extensive research aimed at elucidating the numerous functions of its large multifaceted protein product. While ATM has both nuclear and cytoplasmic functions, this review will focus on its roles in the nucleus where it plays a central role in the very early stages of damage detection and serves as a master controller of cellular responses to DSBs. By activating key regulators of multiple signal transduction pathways, ATM mediates the efficient induction of a signaling network responsible for repair of the damage, and for cellular recovery and survival.

摘要

ATM蛋白激酶是与多效性隐性疾病共济失调毛细血管扩张症相关基因的产物。ATM缺陷细胞对产生DNA双链断裂(DSB)的基因毒性试剂(如电离辐射和放射模拟化学物质)表现出增强的敏感性和大大降低的反应,但对其他试剂诱导的DNA加合物和碱基修饰表现出正常反应。因此,DSB很可能是激活ATM介导途径的主要信号。ATM基因的鉴定引发了广泛的研究,旨在阐明其大型多面蛋白产物的众多功能。虽然ATM具有核和细胞质功能,但本综述将重点关注其在细胞核中的作用,它在损伤检测的非常早期阶段发挥核心作用,并作为细胞对DSB反应的主控制器。通过激活多个信号转导途径的关键调节因子,ATM介导负责损伤修复、细胞恢复和存活的信号网络的有效诱导。

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