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Coordination of DNA Damage Responses via the Smc5/Smc6 Complex

机译:通过Smc5 / Smc6复合体协调DNA损伤反应

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摘要

The detection of DNA damage activates DNA repair pathways and checkpoints to allow time for repair. Ultimately, these responses must be coordinated to ensure that cell cycle progression is halted until repair is completed. Several multiprotein complexes containing members of the structural maintenance of chromosomes family of proteins have been described, including the condensin and cohesin complexes, that are critical for chromosomal organization. Here we show that the Smc5/Smc6 (Smc5/6) complex is required for a coordinated response to DNA damage and normal chromosome integrity. Fission yeast cells lacking functional Smc6 initiate a normal checkpoint response to DNA damage, culminating in the phosphorylation and activation of the Chk1 protein kinase. Despite this, cells enter a lethal mitosis, presumably without completion of DNA repair. Another subunit of the complex, Nse1, is a conserved member of this complex and is also required for this response. We propose that the failure to maintain a checkpoint response stems from the lack of ongoing DNA repair or from defective chromosomal organization, which is the signal to maintain a checkpoint arrest. The Smc5/6 complex is fundamental to genome integrity and may function with the condensin and cohesin complexes in a coordinated manner.
机译:DNA损伤的检测激活了DNA修复途径和检查点,以便有时间进行修复。最终,必须协调这些反应,以确保细胞周期进程中止直至修复完成。已经描述了包含蛋白质的染色体家族的结构维持成员的几种多蛋白复合物,包括凝集素和粘着蛋白复合物,它们对于染色体的组织至关重要。在这里,我们显示Smc5 / Smc6(Smc5 / 6)复杂是对DNA损伤和正常染色体完整性的协调反应所必需的。缺乏功能性Smc6的裂变酵母细胞会启动对DNA损伤的正常检查点反应,最终导致Chk1蛋白激酶的磷酸化和激活。尽管如此,细胞仍可能进入致命的有丝分裂状态,大概是没有完成DNA修复。复合体的另一个子单元Nse1是该复合体的保守成员,也是此响应所必需的。我们认为不能维持检查点反应的原因是缺乏正在进行的DNA修复或染色体组织缺陷,这是维持检查点停滞的信号。 Smc5 / 6复合物是基因组完整性的基础,并且可以与凝聚素和粘附素复合物协同作用。

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