Cancer Cell Laboratory, Department of Biological Sciences, 4401 University Drive, University of Lethbridge, Lethbridge, AB, Canada, T1K 3M4.
Biochem J. 2012 Sep 15;446(3):373-81. doi: 10.1042/BJ20120385.
In the present paper, we report that mitosis is a key step in the cellular response to genotoxic agents in human cells. Cells with damaged DNA recruit γH2AX (phosphorylated histone H2AX), phosphorylate Chk1 (checkpoint kinase 1) and arrest in the G2-phase of the cell cycle. Strikingly, nearly all cells escape the DNA damage checkpoint and become rounded, by a mechanism that correlates with Chk1 dephosphorylation. The rounded cells are alive and in mitosis as measured by low phospho-Tyr(15) Cdk1 (cyclin-dependent kinase 1), high Cdk activity, active Plk1 (Polo-like kinase 1) and high phospho-histone H3 signals. This phenomenon is independent of the type of DNA damage, but is dependent on pharmacologically relevant doses of genotoxicity. Entry into mitosis is likely to be caused by checkpoint adaptation, and the HT-29 cell-based model provides a powerful experimental system in which to explore its molecular basis. We propose that mitosis with damaged DNA is a biologically significant event because it may cause genomic rearrangement in cells that survive genotoxic damage.
在本研究中,我们报告有丝分裂是人类细胞对遗传毒性药物产生细胞反应的关键步骤。有 DNA 损伤的细胞募集 γH2AX(磷酸化组蛋白 H2AX),磷酸化 Chk1(检查点激酶 1)并在细胞周期的 G2 期停滞。引人注目的是,几乎所有细胞都通过与 Chk1 去磷酸化相关的机制逃避了 DNA 损伤检查点,变得圆球状。通过低磷酸化 Tyr(15)Cdk1(周期蛋白依赖性激酶 1)、高 Cdk 活性、活性 Plk1(Polo 样激酶 1)和高磷酸化组蛋白 H3 信号来测量,这些圆球状细胞是存活并处于有丝分裂状态的。这种现象与 DNA 损伤的类型无关,但与遗传毒性的药理学相关剂量有关。进入有丝分裂可能是由检查点适应引起的,而 HT-29 细胞模型提供了一个强大的实验系统,可以用来探索其分子基础。我们提出,带有 DNA 损伤的有丝分裂是一个具有生物学意义的事件,因为它可能导致在遗传毒性损伤后存活的细胞中的基因组重排。
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