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翻译抑制外源性靶RNA介导的微小RNA降解。

Translation suppresses exogenous target RNA-mediated microRNA decay.

作者信息

Li Tianqi, Li Lu, Hiers Nicholas M, Sheng Peike, Wang Yuzhi, Traugot Conner M, Effinger-Morris Jessi F, Akaphan Pitchaporn, Liu Yanyan, Bian Jiang, Fujii Kotaro, Xie Mingyi

机构信息

Department of Biochemistry and Molecular Biology, University of Florida, Gainesville, FL, 32610, USA.

UF Health Cancer Center, University of Florida, Gainesville, FL, 32610, USA.

出版信息

Nat Commun. 2025 Jun 6;16(1):5257. doi: 10.1038/s41467-025-60374-4.

Abstract

MicroRNAs (miRNAs) interact with the target mRNAs to induce translational repression and mRNA degradation. Interestingly, miRNAs themselves can turnover rapidly when binding to a target RNA with extensive complementarity, a phenomenon called target-directed miRNA degradation (TDMD). To date, all validated TDMD "triggers" can induce miRNA degradation reside in non-coding regions of the RNA. We found that TDMD triggers placed in the 3' untranslated region (UTR) of a reporter degraded miRNAs more effectively than those in the coding sequence (CDS). Inhibiting translation of the reporter enhanced miRNA degradation by the CDS trigger, indicating that ribosome-free CDS triggers are more accessible to miRNAs. By small RNA sequencing, we explored mammalian miRNAs sensitive to global translation status. Yet, no endogenous CDS trigger could be confidently assigned to these miRNAs. Our work revealed the intricate relationship between translation and TDMD, and explains the paucity of effective TDMD triggers in the CDS.

摘要

微小RNA(miRNA)与靶mRNA相互作用,以诱导翻译抑制和mRNA降解。有趣的是,当miRNA与具有广泛互补性的靶RNA结合时,其自身会迅速周转,这种现象称为靶标导向的miRNA降解(TDMD)。迄今为止,所有经过验证的能诱导miRNA降解的TDMD“触发因素”都存在于RNA的非编码区域。我们发现,置于报告基因3'非翻译区(UTR)的TDMD触发因素比编码序列(CDS)中的触发因素更有效地降解miRNA。抑制报告基因的翻译可增强CDS触发因素对miRNA的降解作用,这表明无核糖体的CDS触发因素对miRNA更易接近。通过小RNA测序,我们探索了对整体翻译状态敏感的哺乳动物miRNA。然而,尚无内源性CDS触发因素能确切地归因于这些miRNA。我们的工作揭示了翻译与TDMD之间的复杂关系,并解释了CDS中有效TDMD触发因素的匮乏。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3112/12144122/83badd9d533c/41467_2025_60374_Fig1_HTML.jpg

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