Wakeman Timothy P, Xu Bo
Department of Genetics and Stanley S. Scott Cancer Center, LSU Health Sciences Center, New Orleans, LA 70112, United States.
Mutat Res. 2006 Nov 7;610(1-2):14-20. doi: 10.1016/j.mrgentox.2006.06.007. Epub 2006 Jul 27.
Hexavalent chromium (Cr[VI]) is an industrial waste product known to cause nasal and lung cancer in exposed workers. Intracellularly, Cr[VI] undergoes a series of enzymatic reductions resulting in the formation of reactive chromate intermediates and oxygen free radicals. These metabolites react with DNA to cause numerous types of genomic lesions, but the cellular response to these genotoxic insults is poorly understood. Recently, we demonstrated that in response to DNA damage induced by Cr[VI], an ataxia-telangiectasia mutated (ATM) and structural maintenance of chromosomal protein 1 (SMC1)-dependent S-phase checkpoint is activated. Interestingly, this checkpoint response was only ATM-dependent in cells exposed to low doses of Cr[VI], we demonstrate that the ATM and Rad3 related kinase, ATR, is required to activate the S-phase checkpoint. In response to all doses of Cr[VI], ATR is activated and phosphorylates SMC1 to facilitate the checkpoint. Further, chromatin binding ability of Rad17 is required for this process. Taken together, these results indicate that the Rad17-ATR-SMC1 pathway is essential for Cr[VI]-induced S-phase checkpoint activation.
六价铬(Cr[VI])是一种工业废品,已知会导致接触该物质的工人患鼻癌和肺癌。在细胞内,Cr[VI]会经历一系列酶促还原反应,生成具有反应活性的铬酸盐中间体和氧自由基。这些代谢产物与DNA发生反应,导致多种类型的基因组损伤,但细胞对这些基因毒性损伤的反应却知之甚少。最近,我们证明,针对由Cr[VI]诱导的DNA损伤,一种共济失调毛细血管扩张症突变(ATM)和染色体结构维持蛋白1(SMC1)依赖性的S期检查点被激活。有趣的是,这种检查点反应在暴露于低剂量Cr[VI]的细胞中仅依赖ATM,我们证明ATM和Rad3相关激酶ATR对于激活S期检查点是必需的。针对所有剂量的Cr[VI],ATR都会被激活并使SMC1磷酸化,以促进检查点的作用。此外,该过程需要Rad17的染色质结合能力。综上所述,这些结果表明Rad17-ATR-SMC1途径对于Cr[VI]诱导的S期检查点激活至关重要。
