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DHX9 应激颗粒对 RNA 损伤的区室化。

RNA damage compartmentalization by DHX9 stress granules.

机构信息

Max Planck Institute of Immunobiology and Epigenetics, Freiburg, Germany.

EMcore, Renal Division, Department of Medicine, University Freiburg, Hospital Freiburg, University Faculty of Medicine, Freiburg, Germany.

出版信息

Cell. 2024 Mar 28;187(7):1701-1718.e28. doi: 10.1016/j.cell.2024.02.028. Epub 2024 Mar 18.

Abstract

Biomolecules incur damage during stress conditions, and damage partitioning represents a vital survival strategy for cells. Here, we identified a distinct stress granule (SG), marked by dsRNA helicase DHX9, which compartmentalizes ultraviolet (UV)-induced RNA, but not DNA, damage. Our FANCI technology revealed that DHX9 SGs are enriched in damaged intron RNA, in contrast to classical SGs that are composed of mature mRNA. UV exposure causes RNA crosslinking damage, impedes intron splicing and decay, and triggers DHX9 SGs within daughter cells. DHX9 SGs promote cell survival and induce dsRNA-related immune response and translation shutdown, differentiating them from classical SGs that assemble downstream of translation arrest. DHX9 modulates dsRNA abundance in the DHX9 SGs and promotes cell viability. Autophagy receptor p62 is activated and important for DHX9 SG disassembly. Our findings establish non-canonical DHX9 SGs as a dedicated non-membrane-bound cytoplasmic compartment that safeguards daughter cells from parental RNA damage.

摘要

生物分子在应激条件下会受到损伤,而损伤分区代表了细胞的一种重要生存策略。在这里,我们鉴定出一种由双链 RNA 解旋酶 DHX9 标记的独特应激颗粒(SG),它将紫外线(UV)诱导的 RNA ,而不是 DNA ,损伤进行区室化。我们的 FANCI 技术揭示,DHX9 SGs 富含受损的内含子 RNA,而不同于由成熟 mRNA 组成的经典 SG。UV 暴露会导致 RNA 交联损伤,阻碍内含子剪接和降解,并在子细胞中引发 DHX9 SGs。DHX9 SGs 促进细胞存活,并诱导 dsRNA 相关免疫反应和翻译关闭,使其与在翻译抑制下游组装的经典 SG 区分开来。DHX9 调节 DHX9 SG 中的 dsRNA 丰度并促进细胞活力。自噬受体 p62 被激活,对于 DHX9 SG 的解体很重要。我们的发现确立了非典型的 DHX9 SG 作为一种专门的非膜结合细胞质隔室,可保护子细胞免受亲本 RNA 损伤。

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