分子伴侣 ALYREF 可促进 R 环的解析并保持基因组的稳定性。

IF 4 2区 生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
Jay Bhandari, Cristina Guillén-Mendoza, Kathryn Banks, Lillian Eliaz, Sierra Southwell, Darriel Eyaa, Rosa Luna, Andrés Aguilera, Xiaoyu Xue
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引用次数: 0

摘要

计划外的 R 环通常会造成 DNA 损伤和复制压力,因此是基因组稳定性的主要威胁。一些 RNA 处理因子,包括保守的 THO 复合物及其相关的 RNA 和 DNA-RNA 螺旋酶 UAP56,可防止细胞中 R 环的积累。在此,我们研究了与 UAP56 和 THO 复合物相关的 RNA 导出适配器 ALYREF 在 R 环调控中的功能。我们证明纯化的 ALYREF 在体外能促进 UAP56 介导的 R 环解离,这种刺激依赖于它与 UAP56 和 R 环的相互作用。重要的是,我们发现 ALYREF 能结合 DNA-RNA 杂交体和 R 环。同样,ALYREF 的耗竭会导致细胞中 R 环的积累和 R 环介导的基因组不稳定性。我们认为,ALYREF 除了在 RNA 代谢和导出中的已知作用外,还是一个关键的细胞 R 环协同调节器,它能结合 R 环,并在转录过程中刺激 UAP56 驱动的非调度 R 环的解析。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The molecular chaperone ALYREF promotes R-loop resolution and maintains genome stability.

Unscheduled R-loops usually cause DNA damage and replication stress, and are therefore a major threat to genome stability. Several RNA processing factors, including the conserved THO complex and its associated RNA and DNA-RNA helicase UAP56, prevent R-loop accumulation in cells. Here we investigate the function of ALYREF, an RNA export adapter associated with UAP56 and the THO complex, in R-loop regulation. We demonstrate that purified ALYREF promotes UAP56-mediated R-loop dissociation in vitro, and this stimulation is dependent on its interaction with UAP56 and R-loops. Importantly, we show that ALYREF binds DNA-RNA hybrids and R-loops. Consistently, ALYREF depletion causes R-loop accumulation and R-loop-mediated genome instability in cells. We propose that ALYREF, apart from its known role in RNA metabolism and export, is a key cellular R-loop co-regulator, which binds R-loops and stimulates UAP56-driven resolution of unscheduled R-loops during transcription.

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来源期刊
Journal of Biological Chemistry
Journal of Biological Chemistry Biochemistry, Genetics and Molecular Biology-Biochemistry
自引率
4.20%
发文量
1233
期刊介绍: The Journal of Biological Chemistry welcomes high-quality science that seeks to elucidate the molecular and cellular basis of biological processes. Papers published in JBC can therefore fall under the umbrellas of not only biological chemistry, chemical biology, or biochemistry, but also allied disciplines such as biophysics, systems biology, RNA biology, immunology, microbiology, neurobiology, epigenetics, computational biology, ’omics, and many more. The outcome of our focus on papers that contribute novel and important mechanistic insights, rather than on a particular topic area, is that JBC is truly a melting pot for scientists across disciplines. In addition, JBC welcomes papers that describe methods that will help scientists push their biochemical inquiries forward and resources that will be of use to the research community.
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