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The Chromatin Scaffold Protein SAFB1 Renders Chromatin Permissive for DNA Damage Signaling

机译:染色质支架蛋白SAFB1使染色质允许DNA损伤信号转导

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摘要

Although the general relevance of chromatin modifications for genotoxic stress signaling, cell-cycle checkpoint activation, and DNA repair is well established, how these modifications reach initial thresholds in order to trigger robust responses remains largely unexplored. Here, we identify the chromatin-associated scaffold attachment factor SAFB1 as a component of the DNA damage response and show that SAFB1 cooperates with histone acetylation to allow for efficient γH2AX spreading and genotoxic stress signaling. SAFB1 undergoes a highly dynamic exchange at damaged chromatin in a poly(ADP-ribose)-polymerase 1- and poly(ADP-ribose)-dependent manner and is required for unperturbed cell-cycle checkpoint activation and guarding cells against replicative stress. Altogether, our data reveal that transient recruitment of an architectural chromatin component is required in order to overcome physiological barriers by making chromatin permissive for DNA damage signaling, whereas the ensuing exclusion of SAFB1 may help prevent excessive signaling.
机译:尽管已经很好地确定了染色质修饰与遗传毒性应激信号转导,细胞周期检查点激活和DNA修复的一般相关性,但这些修饰如何达到初始阈值以触发鲁棒应答仍然没有被广泛研究。在这里,我们确定了染色质相关的支架附着因子SAFB1作为DNA损伤反应的一个组成部分,并表明SAFB1与组蛋白乙酰化协同作用以实现有效的γH2AX扩散和遗传毒性应激信号传递。 SAFB1以聚(ADP-核糖)-聚合酶1-和聚(ADP-核糖)依赖性方式在受损的染色质上进行高度动态交换,是不受干扰的细胞周期检查点激活和保护细胞免受复制压力的必需条件。总而言之,我们的数据表明,通过使染色质对DNA损伤信号而言是允许的,需要短暂募集建筑染色质成分才能克服生理障碍,而随后排斥SAFB1则可能有助于防止过度的信号传导。

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