BRCA1-Ku80 蛋白相互作用增强了细胞周期 G1 期染色体双链断裂的末端连接保真度。
BRCA1-Ku80 protein interaction enhances end-joining fidelity of chromosomal double-strand breaks in the G1 phase of the cell cycle.
机构信息
Department of Radiation Oncology, The Ohio State University Medical Center, Arthur G. James Comprehensive Cancer Center, Columbus, OH 43210, USA.
出版信息
J Biol Chem. 2013 Mar 29;288(13):8966-76. doi: 10.1074/jbc.M112.412650. Epub 2013 Jan 23.
Abstract
Quality control of DNA double-strand break (DSB) repair is vital in preventing mutagenesis. Non-homologous end-joining (NHEJ), a repair process predominant in the G1 phase of the cell cycle, rejoins DSBs either accurately or with errors, but the mechanisms controlling its fidelity are poorly understood. Here we show that BRCA1, a tumor suppressor, enhances the fidelity of NHEJ-mediated DSB repair and prevents mutagenic deletional end-joining through interaction with canonical NHEJ machinery during G1. BRCA1 binds and stabilizes Ku80 at DSBs through its N-terminal region, promotes precise DSB rejoining, and increases cellular resistance to radiation-induced DNA damage in a G1 phase-specific manner. These results suggest that BRCA1, as a central player in genome integrity maintenance, ensures high fidelity repair of DSBs by not only promoting homologous recombination repair in G2/M phase but also facilitating fidelity of Ku80-dependent NHEJ repair, thus preventing deletional end-joining of chromosomal DSBs during G1.
摘要
DNA 双链断裂 (DSB) 修复的质量控制对于防止突变至关重要。非同源末端连接 (NHEJ) 是细胞周期 G1 期主要的修复过程,它可以准确或错误地连接 DSB,但控制其保真度的机制还知之甚少。本文作者表明,肿瘤抑制因子 BRCA1 通过与 G1 期的经典 NHEJ 机制相互作用,增强 NHEJ 介导的 DSB 修复的保真度,并防止突变性缺失性末端连接。BRCA1 通过其 N 端区域与 Ku80 结合并稳定 DSB,促进精确的 DSB 连接,并以 G1 期特异性方式增加细胞对辐射诱导的 DNA 损伤的抗性。这些结果表明,BRCA1 作为基因组完整性维持的核心参与者,不仅通过促进 G2/M 期的同源重组修复,而且通过促进 Ku80 依赖性 NHEJ 修复的保真度,确保 DSB 的高保真修复,从而防止 G1 期染色体 DSB 的缺失性末端连接。
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