急性MUS81缺失导致复制叉减慢和持续性DNA损伤反应。

Acute MUS81 depletion leads to replication fork slowing and a constitutive DNA damage response.

作者信息

Xing Meichun, Wang Xiaohui, Palmai-Pallag Timea, Shen Huahao, Helleday Thomas, Hickson Ian D, Ying Songmin

机构信息

Department of Pharmacology, Zhejiang University School of Medicine, Hangzhou, China.

School of Life Sciences, University of Lincoln, Lincoln, United Kingdom.

出版信息

Oncotarget. 2015 Nov 10;6(35):37638-46. doi: 10.18632/oncotarget.5497.

DOI:10.18632/oncotarget.5497

PMID:26415217

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4741954/

Abstract

The MUS81 protein belongs to a conserved family of DNA structure-specific nucleases that play important roles in DNA replication and repair. Inactivation of the Mus81 gene in mice has no major deleterious consequences for embryonic development, although cancer susceptibility has been reported. We have investigated the role of MUS81 in human cells by acutely depleting the protein using shRNAs. We found that MUS81 depletion from human fibroblasts leads to accumulation of ssDNA and a constitutive DNA damage response that ultimately activates cellular senescence. Moreover, we show that MUS81 is required for efficient replication fork progression during an unperturbed S-phase, and for recovery of productive replication following replication stalling. These results demonstrate essential roles for the MUS81 nuclease in maintenance of replication fork integrity.

摘要

MUS81蛋白属于一个保守的DNA结构特异性核酸酶家族，在DNA复制和修复中发挥重要作用。尽管有报道称Mus81基因失活的小鼠对胚胎发育没有重大有害影响，但对癌症易感性有影响。我们通过使用短发夹RNA（shRNAs）急性消耗该蛋白，研究了MUS81在人类细胞中的作用。我们发现，从人类成纤维细胞中去除MUS81会导致单链DNA积累和持续性DNA损伤反应，最终激活细胞衰老。此外，我们表明，在未受干扰的S期，高效的复制叉进展以及复制停滞后恢复有活性的复制都需要MUS81。这些结果证明了MUS81核酸酶在维持复制叉完整性中的重要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f401/4741954/5747d19c6713/oncotarget-06-37638-g001.jpg

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急性MUS81缺失导致复制叉减慢和持续性DNA损伤反应。

Acute MUS81 depletion leads to replication fork slowing and a constitutive DNA damage response.

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