Lou Zhenkun, Chini Claudia Christiano Silva, Minter-Dykhouse Katherine, Chen Junjie
Department of Oncology, Mayo Clinic and Foundation, Rochester, Minnesota 55905, USA.
J Biol Chem. 2003 Apr 18;278(16):13599-602. doi: 10.1074/jbc.C300060200. Epub 2003 Feb 27.
BRCA1 is a tumor suppressor involved in DNA repair and damage-induced checkpoint controls. In response to DNA damage, BRCA1 relocalizes to nuclear foci at the sites of DNA lesions. However, little is known about the regulation of BRCA1 relocalization following DNA damage. Here we show that mediator of DNA damage checkpoint protein 1 (MDC1), previously named NFBD1 or Kiaa0170, is a proximate mediator of DNA damage responses that regulates BRCA1 function. MDC1 regulates ataxia-telangiectasia-mutated (ATM)-dependent phosphorylation events at the site of DNA damage. Importantly down-regulation of MDC1 abolishes the relocalization and hyperphosphorylation of BRCA1 following DNA damage, which coincides with defective G(2)/M checkpoint control in response to DNA damage. Taken together these data suggest that MDC1 regulates BRCA1 function in DNA damage checkpoint control.
BRCA1是一种参与DNA修复和损伤诱导的检查点控制的肿瘤抑制因子。响应DNA损伤时,BRCA1会重新定位到DNA损伤位点的核病灶处。然而,关于DNA损伤后BRCA1重新定位的调控机制知之甚少。在此我们表明,DNA损伤检查点蛋白1(MDC1,先前称为NFBD1或Kiaa0170)是调节BRCA1功能的DNA损伤反应的直接介导因子。MDC1在DNA损伤位点调节共济失调毛细血管扩张症突变(ATM)依赖性磷酸化事件。重要的是,MDC1的下调消除了DNA损伤后BRCA1的重新定位和过度磷酸化,这与响应DNA损伤时G(2)/M检查点控制缺陷相吻合。综合这些数据表明,MDC1在DNA损伤检查点控制中调节BRCA1的功能。
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