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RNA 5-甲基胞嘧啶标记线粒体双链 RNA 进行降解并释放到细胞质中。

RNA 5-methylcytosine marks mitochondrial double-stranded RNAs for degradation and cytosolic release.

机构信息

Department of Chemical and Biomolecular Engineering, Korea Advanced Institute of Science and Technology (KAIST), Daejeon 34141, Republic of Korea.

Xaira Therapeutics, Foster City, CA 94404, USA.

出版信息

Mol Cell. 2024 Aug 8;84(15):2935-2948.e7. doi: 10.1016/j.molcel.2024.06.023. Epub 2024 Jul 16.

DOI:10.1016/j.molcel.2024.06.023
PMID:39019044
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11316625/
Abstract

Mitochondria are essential regulators of innate immunity. They generate long mitochondrial double-stranded RNAs (mt-dsRNAs) and release them into the cytosol to trigger an immune response under pathological stress conditions. Yet the regulation of these self-immunogenic RNAs remains largely unknown. Here, we employ CRISPR screening on mitochondrial RNA (mtRNA)-binding proteins and identify NOP2/Sun RNA methyltransferase 4 (NSUN4) as a key regulator of mt-dsRNA expression in human cells. We find that NSUN4 induces 5-methylcytosine (mC) modification on mtRNAs, especially on the termini of light-strand long noncoding RNAs. These mC-modified RNAs are recognized by complement C1q-binding protein (C1QBP), which recruits polyribonucleotide nucleotidyltransferase to facilitate RNA turnover. Suppression of NSUN4 or C1QBP results in increased mt-dsRNA expression, while C1QBP deficiency also leads to increased cytosolic mt-dsRNAs and subsequent immune activation. Collectively, our study unveils the mechanism underlying the selective degradation of light-strand mtRNAs and establishes a molecular mark for mtRNA decay and cytosolic release.

摘要

线粒体是先天免疫的重要调节因子。它们产生长的线粒体双链 RNA(mt-dsRNA),并将其释放到细胞质中,在病理应激条件下引发免疫反应。然而,这些自身免疫性 RNA 的调节在很大程度上仍然未知。在这里,我们通过 CRISPR 筛选线粒体 RNA(mtRNA)结合蛋白,并鉴定出 NOP2/Sun RNA 甲基转移酶 4(NSUN4)是人类细胞中 mt-dsRNA 表达的关键调节因子。我们发现 NSUN4 诱导 mtRNA 上的 5-甲基胞嘧啶(mC)修饰,特别是在轻链长非编码 RNA 的末端。这些 mC 修饰的 RNA 被补体 C1q 结合蛋白(C1QBP)识别,C1QBP 招募多核苷酸核苷酸转移酶以促进 RNA 周转。抑制 NSUN4 或 C1QBP 会导致 mt-dsRNA 表达增加,而 C1QBP 缺陷也会导致细胞质中 mt-dsRNA 增加和随后的免疫激活。总之,我们的研究揭示了轻链 mtRNA 选择性降解的机制,并为 mtRNA 降解和细胞质释放建立了分子标记。

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