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人类细胞中 THO/TREX 缺失导致基因组不稳定和转录延伸损伤。

Genome instability and transcription elongation impairment in human cells depleted of THO/TREX.

机构信息

Centro Andaluz de Biología Molecular y Medicina Regenerativa (CABIMER), Universidad de Sevilla - Consejo Superior de Investigaciones Científicas (CSIC), Sevilla, Spain.

出版信息

PLoS Genet. 2011 Dec;7(12):e1002386. doi: 10.1371/journal.pgen.1002386. Epub 2011 Dec 1.

Abstract

THO/TREX connects transcription with genome integrity in yeast, but a role of mammalian THO in these processes is uncertain, which suggests a differential implication of mRNP biogenesis factors in genome integrity in yeast and humans. We show that human THO depletion impairs transcription elongation and mRNA export and increases instability associated with DNA breaks, leading to hyper-recombination and γH2AX and 53BP1 foci accumulation. This is accompanied by replication alteration as determined by DNA combing. Genome instability is R-loop-dependent, as deduced from the ability of the AID enzyme to increase DNA damage and of RNaseH to reduce it, or from the enhancement of R-loop-dependent class-switching caused by THOC1-depletion in CH12 murine cells. Therefore, mammalian THO prevents R-loop formation and has a role in genome dynamics and function consistent with an evolutionary conservation of the functional connection between these mRNP biogenesis factors and genome integrity that had not been anticipated.

摘要

THO/TREX 在酵母中连接转录与基因组完整性,但哺乳动物 THO 在这些过程中的作用尚不确定,这表明在酵母和人类中,mRNA 生物发生因子对基因组完整性的影响存在差异。我们发现,人类 THO 耗竭会损害转录延伸和 mRNA 输出,并增加与 DNA 断裂相关的不稳定性,导致超重组和 γH2AX 和 53BP1 焦点积累。这伴随着 DNA 梳理确定的复制改变。基因组不稳定性是 R 环依赖性的,这可以从 AID 酶增加 DNA 损伤的能力和 RNaseH 降低其损伤的能力推断出来,或者从 CH12 鼠细胞中 THOC1 耗竭引起的 R 环依赖性类别转换增强推断出来。因此,哺乳动物 THO 可防止 R 环形成,并在基因组动态和功能中发挥作用,这与这些 mRNP 生物发生因子与基因组完整性之间的功能连接的进化保守性一致,而这是之前未曾预料到的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4084/3228816/2da7814638b2/pgen.1002386.g001.jpg

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