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一种构象变化的核酸酶解开结构 RNA。

A shape-shifting nuclease unravels structured RNA.

机构信息

W.M. Keck Structural Biology Laboratory, Howard Hughes Medical Institute, New York, NY, USA.

School of Biological Sciences, Cold Spring Harbor Laboratory, New York, NY, USA.

出版信息

Nat Struct Mol Biol. 2023 Mar;30(3):339-347. doi: 10.1038/s41594-023-00923-x. Epub 2023 Feb 23.

Abstract

RNA turnover pathways ensure appropriate gene expression levels by eliminating unwanted transcripts. Dis3-like 2 (Dis3L2) is a 3'-5' exoribonuclease that plays a critical role in human development. Dis3L2 independently degrades structured substrates, including coding and noncoding 3' uridylated RNAs. While the basis for Dis3L2's substrate recognition has been well characterized, the mechanism of structured RNA degradation by this family of enzymes is unknown. We characterized the discrete steps of the degradation cycle by determining cryogenic electron microscopy structures representing snapshots along the RNA turnover pathway and measuring kinetic parameters for RNA processing. We discovered a dramatic conformational change that is triggered by double-stranded RNA (dsRNA), repositioning two cold shock domains by 70 Å. This movement exposes a trihelix linker region, which acts as a wedge to separate the two RNA strands. Furthermore, we show that the trihelix linker is critical for dsRNA, but not single-stranded RNA, degradation. These findings reveal the conformational plasticity of Dis3L2 and detail a mechanism of structured RNA degradation.

摘要

RNA 周转途径通过消除不需要的转录本来确保适当的基因表达水平。Dis3 样 2(Dis3L2)是一种 3'-5'外切核酸酶,在人类发育中起着关键作用。Dis3L2 可独立降解结构底物,包括编码和非编码的 3'尿苷化 RNA。虽然 Dis3L2 底物识别的基础已经得到很好的描述,但该酶家族对结构 RNA 降解的机制尚不清楚。我们通过确定代表 RNA 周转途径中各个步骤的低温电子显微镜结构并测量 RNA 处理的动力学参数,来表征降解循环的离散步骤。我们发现了一种由双链 RNA(dsRNA)触发的剧烈构象变化,该变化使两个冷休克结构域重新定位 70Å。这种运动暴露了一个三联螺旋连接区,它充当楔子将两个 RNA 链分开。此外,我们表明三联螺旋连接区对于 dsRNA,但不是单链 RNA 的降解至关重要。这些发现揭示了 Dis3L2 的构象灵活性,并详细说明了一种结构 RNA 降解的机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7147/10023572/327e573fdb7c/41594_2023_923_Fig1_HTML.jpg

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