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mRNA 加帽酶定位于细胞质中的应激颗粒中,并维持靶 mRNA 的帽状结构的平衡。

The mRNA-capping enzyme localizes to stress granules in the cytoplasm and maintains cap homeostasis of target mRNAs.

机构信息

RNABio Lab, Institute of Health Sciences, Presidency University, Kolkata, West Bengal 700156, India.

CellBio Lab, Institute of Health Sciences, Presidency University, Kolkata, West Bengal 700156, India.

出版信息

J Cell Sci. 2024 Jun 1;137(11). doi: 10.1242/jcs.261578. Epub 2024 Jun 6.

DOI:10.1242/jcs.261578
PMID:38841902
Abstract

The model of RNA stability has undergone a transformative shift with the revelation of a cytoplasmic capping activity that means a subset of transcripts are recapped autonomously of their nuclear counterparts. The present study demonstrates nucleo-cytoplasmic shuttling of the mRNA-capping enzyme (CE, also known as RNA guanylyltransferase and 5'-phosphatase; RNGTT), traditionally acknowledged for its nuclear localization and functions, elucidating its contribution to cytoplasmic capping activities. A unique nuclear export sequence in CE mediates XPO1-dependent nuclear export of CE. Notably, during sodium arsenite-induced oxidative stress, cytoplasmic CE (cCE) congregates within stress granules (SGs). Through an integrated approach involving molecular docking and subsequent co-immunoprecipitation, we identify eIF3b, a constituent of SGs, as an interactive associate of CE, implying that it has a potential role in guiding cCE to SGs. We measured the cap status of specific mRNA transcripts from U2OS cells that were non-stressed, stressed and recovered from stress, which indicated that cCE-target transcripts lost their caps during stress but remarkably regained cap stability during the recovery phase. This comprehensive study thus uncovers a novel facet of cytoplasmic CE, which facilitates cellular recovery from stress by maintaining cap homeostasis of target mRNAs.

摘要

RNA 稳定性模型发生了重大转变,揭示了细胞质加帽活性,这意味着一部分转录本可以在与核对应物无关的情况下自主加帽。本研究证明了 mRNA 加帽酶 (CE,也称为 RNA 鸟苷转移酶和 5'-磷酸酶;RNGTT) 的核质穿梭,CE 传统上被认为定位于细胞核并具有核功能,阐明了其对细胞质加帽活性的贡献。CE 中的一个独特的核输出序列介导了 XPO1 依赖性的 CE 核输出。值得注意的是,在亚砷酸钠诱导的氧化应激期间,细胞质 CE(cCE)聚集在应激颗粒(SGs)中。通过涉及分子对接和随后的共免疫沉淀的综合方法,我们鉴定出 SGs 的组成部分 eIF3b 是 CE 的相互作用伴侣,这意味着它在指导 cCE 到 SGs 中具有潜在作用。我们测量了非应激、应激和应激恢复的 U2OS 细胞中特定 mRNA 转录本的帽状态,结果表明 cCE 靶向的转录本在应激期间失去了帽,但在恢复阶段显著恢复了帽稳定性。这项全面的研究因此揭示了细胞质 CE 的一个新方面,它通过维持靶 mRNA 的帽稳态促进细胞从应激中恢复。

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