Institute of Cancer Biology and Centre for Genotoxic Stress Research, Danish Cancer Society, DK-2100 Copenhagen, Denmark.
J Cell Biol. 2010 Sep 6;190(5):731-40. doi: 10.1083/jcb.200912135. Epub 2010 Aug 30.
In response to ionizing radiation (IR), cells delay cell cycle progression and activate DNA repair. Both processes are vital for genome integrity, but the mechanisms involved in their coordination are not fully understood. In a mass spectrometry screen, we identified the adenosine triphosphate-dependent chromatin-remodeling protein CHD4 (chromodomain helicase DNA-binding protein 4) as a factor that becomes transiently immobilized on chromatin after IR. Knockdown of CHD4 triggers enhanced Cdc25A degradation and p21(Cip1) accumulation, which lead to more pronounced cyclin-dependent kinase inhibition and extended cell cycle delay. At DNA double-strand breaks, depletion of CHD4 disrupts the chromatin response at the level of the RNF168 ubiquitin ligase, which in turn impairs local ubiquitylation and BRCA1 assembly. These cell cycle and chromatin defects are accompanied by elevated spontaneous and IR-induced DNA breakage, reduced efficiency of DNA repair, and decreased clonogenic survival. Thus, CHD4 emerges as a novel genome caretaker and a factor that facilitates both checkpoint signaling and repair events after DNA damage.
针对电离辐射 (IR),细胞会延迟细胞周期进程并激活 DNA 修复。这两个过程对于基因组完整性至关重要,但它们协调的机制尚未完全了解。在一项质谱筛选中,我们发现三磷酸腺苷依赖性染色质重塑蛋白 CHD4(染色质螺旋酶 DNA 结合蛋白 4)是一种在受到 IR 后会短暂固定在染色质上的因子。CHD4 的敲低会触发 Cdc25A 降解和 p21(Cip1)积累增强,导致更明显的细胞周期蛋白依赖性激酶抑制和细胞周期延长。在 DNA 双链断裂处,CHD4 的耗竭会破坏 RNF168 泛素连接酶水平的染色质反应,进而损害局部泛素化和 BRCA1 组装。这些细胞周期和染色质缺陷伴随着自发和 IR 诱导的 DNA 断裂增加、DNA 修复效率降低和集落形成能力降低。因此,CHD4 成为一种新的基因组守护者,有助于 DNA 损伤后检查点信号和修复事件的发生。
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