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RNA 代谢是甲酰胺在体内的主要靶标。

RNA metabolism is the primary target of formamide in vivo.

机构信息

Centro Andaluz de Biología del Desarrollo, Universidad Pablo de Olavide/Consejo Superior de Investigaciones Científicas, Carretera de Utrera Km1, 41013, Seville, Spain.

Research Department of Genetics, Evolution and Environment and UCL Institute of Healthy Ageing, University College London, WC1E 6BT, London, United Kingdom.

出版信息

Sci Rep. 2017 Nov 21;7(1):15895. doi: 10.1038/s41598-017-16291-8.

Abstract

The synthesis, processing and function of coding and non-coding RNA molecules and their interacting proteins has been the focus of a great deal of research that has boosted our understanding of key molecular pathways that underlie higher order events such as cell cycle control, development, innate immune response and the occurrence of genetic diseases. In this study, we have found that formamide preferentially weakens RNA related processes in vivo. Using a non-essential Schizosaccharomyces pombe gene deletion collection, we identify deleted loci that make cells sensitive to formamide. Sensitive deletions are significantly enriched in genes involved in RNA metabolism. Accordingly, we find that previously known temperature-sensitive splicing mutants become lethal in the presence of the drug under permissive temperature. Furthermore, in a wild type background, splicing efficiency is decreased and R-loop formation is increased in the presence of formamide. In addition, we have also isolated 35 formamide-sensitive mutants, many of which display remarkable morphology and cell cycle defects potentially unveiling new players in the regulation of these processes. We conclude that formamide preferentially targets RNA related processes in vivo, probably by relaxing RNA secondary structures and/or RNA-protein interactions, and can be used as an effective tool to characterize these processes.

摘要

编码和非编码 RNA 分子及其相互作用蛋白的合成、加工和功能一直是大量研究的焦点,这些研究增进了我们对关键分子途径的理解,这些途径是细胞周期控制、发育、先天免疫反应和遗传疾病发生等高级事件的基础。在这项研究中,我们发现甲酰胺在体内优先削弱与 RNA 相关的过程。使用非必需的裂殖酵母基因缺失文库,我们确定了使细胞对甲酰胺敏感的缺失基因座。敏感缺失明显富集在参与 RNA 代谢的基因中。因此,我们发现先前已知的温度敏感剪接突变体在允许温度下存在药物时变得致命。此外,在野生型背景下,甲酰胺的存在会降低剪接效率并增加 R 环形成。此外,我们还分离了 35 种甲酰胺敏感突变体,其中许多表现出明显的形态和细胞周期缺陷,可能揭示了这些过程调节的新参与者。我们得出结论,甲酰胺在体内优先靶向与 RNA 相关的过程,可能通过放松 RNA 二级结构和/或 RNA-蛋白质相互作用,并可作为一种有效的工具来研究这些过程。

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