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RNA 解旋酶 IGHMBP2 通过调控 THO 复合物以确保细胞 mRNA 内稳。

RNA helicase IGHMBP2 regulates THO complex to ensure cellular mRNA homeostasis.

机构信息

Department of Biochemistry 1, Biocenter, University of Würzburg, 97074 Würzburg, Germany.

Department of Biochemistry 1, Biocenter, University of Würzburg, 97074 Würzburg, Germany.

出版信息

Cell Rep. 2024 Feb 27;43(2):113802. doi: 10.1016/j.celrep.2024.113802. Epub 2024 Feb 17.

Abstract

RNA helicases constitute a large protein family implicated in cellular RNA homeostasis and disease development. Here, we show that the RNA helicase IGHMBP2, linked to the neuromuscular disorder spinal muscular atrophy with respiratory distress type 1 (SMARD1), associates with polysomes and impacts translation of mRNAs containing short, GC-rich, and structured 5' UTRs. The absence of IGHMBP2 causes ribosome stalling at the start codon of target mRNAs, leading to reduced translation efficiency. The main mRNA targets of IGHMBP2-mediated regulation encode for components of the THO complex (THOC), linking IGHMBP2 to mRNA production and nuclear export. Accordingly, failure of IGHMBP2 regulation of THOC causes perturbations of the transcriptome and its encoded proteome, and ablation of THOC subunits phenocopies these changes. Thus, IGHMBP2 is an upstream regulator of THOC. Of note, IGHMBP2-dependent regulation of THOC is also observed in astrocytes derived from patients with SMARD1 disease, suggesting that deregulated mRNA metabolism contributes to SMARD1 etiology and may enable alternative therapeutic avenues.

摘要

RNA 解旋酶构成了一个庞大的蛋白质家族,它们与细胞内 RNA 的动态平衡和疾病的发展有关。在这里,我们表明,与神经肌肉疾病伴有呼吸窘迫和运动神经元病 1 型(SMARD1)相关的 RNA 解旋酶IGHMBP2 与多核糖体结合,并影响含有短、GC 丰富和结构 5'UTR 的 mRNAs 的翻译。IGHMBP2 的缺失导致核糖体在靶 mRNAs 的起始密码子处停滞,从而降低翻译效率。IGHMBP2 介导调节的主要 mRNA 靶标编码 THO 复合物(THOC)的组件,将 IGHMBP2 与 mRNA 的产生和核输出联系起来。因此,IGHMBP2 对 THOC 的调节失败导致转录组及其编码的蛋白质组发生扰动,并且 THOC 亚基的缺失模拟了这些变化。因此,IGHMBP2 是 THOC 的上游调节剂。值得注意的是,在源自 SMARD1 疾病患者的星形胶质细胞中也观察到 IGHMBP2 对 THOC 的依赖性调节,这表明失调的 mRNA 代谢有助于 SMARD1 的发病机制,并可能为其他治疗途径提供可能性。

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