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Ddx19 RNA解旋酶在细胞核R环代谢中依赖ATR的功能。

An ATR-dependent function for the Ddx19 RNA helicase in nuclear R-loop metabolism.

作者信息

Hodroj Dana, Recolin Bénédicte, Serhal Kamar, Martinez Susan, Tsanov Nikolay, Abou Merhi Raghida, Maiorano Domenico

机构信息

Genome Surveillance and Stability Laboratory, Institute of Human Genetics, UMR9002, CNRS-UM, University of Montpellier, Montpellier Cedex 5, France.

Genomics and Health Laboratory, Biology Department, Faculty of Sciences, R. Hariri Campus, Lebanese University, Hadath, Lebanon.

出版信息

EMBO J. 2017 May 2;36(9):1182-1198. doi: 10.15252/embj.201695131. Epub 2017 Mar 17.

Abstract

Coordination between transcription and replication is crucial in the maintenance of genome integrity. Disturbance of these processes leads to accumulation of aberrant DNA:RNA hybrids (R-loops) that, if unresolved, generate DNA damage and genomic instability. Here we report a novel, unexpected role for the nucleopore-associated mRNA export factor Ddx19 in removing nuclear R-loops formed upon replication stress or DNA damage. We show, in live cells, that Ddx19 transiently relocalizes from the nucleopore to the nucleus upon DNA damage, in an ATR/Chk1-dependent manner, and that Ddx19 nuclear relocalization is required to clear R-loops. Ddx19 depletion induces R-loop accumulation, proliferation-dependent DNA damage and defects in replication fork progression. Further, we show that Ddx19 resolves R-loops via its helicase activity. Furthermore, mutation of a residue phosphorylated by Chk1 in Ddx19 disrupts its interaction with Nup214 and allows its nuclear relocalization. Finally, we show that Ddx19 operates in resolving R-loops independently of the RNA helicase senataxin. Altogether these observations put forward a novel, ATR-dependent function for Ddx19 in R-loop metabolism to preserve genome integrity in mammalian cells.

摘要

转录与复制之间的协调对于维持基因组完整性至关重要。这些过程的紊乱会导致异常DNA:RNA杂交体(R环)的积累,若不解决,会产生DNA损伤和基因组不稳定。在此,我们报告核孔相关的mRNA输出因子Ddx19在去除复制应激或DNA损伤时形成的核R环方面具有一种新的、意想不到的作用。我们在活细胞中表明,DNA损伤时,Ddx19以ATR/Chk1依赖的方式从核孔短暂重新定位到细胞核,并且Ddx19的核重新定位是清除R环所必需的。Ddx19的缺失会诱导R环积累、增殖依赖性DNA损伤以及复制叉进展缺陷。此外,我们表明Ddx19通过其解旋酶活性解决R环。此外,Ddx19中被Chk1磷酸化的一个残基的突变会破坏其与Nup214的相互作用,并使其核重新定位。最后,我们表明Ddx19在解决R环时独立于RNA解旋酶senataxin发挥作用。总之,这些观察结果提出了Ddx19在R环代谢中一种新的、依赖ATR的功能,以在哺乳动物细胞中维持基因组完整性。

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