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Drosha 介导 Lin28 mRNA 靶标的不稳定化。

Drosha mediates destabilization of Lin28 mRNA targets.

机构信息

Department of Obstetrics, Gynecology and Reproductive Sciences, Yale Stem Cell Center, Yale University School of Medicine, New Haven, CT, USA.

出版信息

Cell Cycle. 2012 Oct 1;11(19):3590-8. doi: 10.4161/cc.21871. Epub 2012 Aug 30.

Abstract

Lin28 plays important roles in development, stem cell maintenance, oncogenesis and metabolism. As an RNA-binding protein, it blocks the biogenesis primarily of let-7 family miRNAs and also promotes translation of a cohort of mRNAs involved in cell growth, metabolism and pluripotency, likely through recognition of distinct sequence and structural motifs within mRNAs. Here, we show that one such motif, shared by multiple Lin28-responsive elements (LREs) present in Lin28 mRNA targets also participates in a Drosha-dependent regulation and may contribute to destabilization of its cognate mRNAs. We further show that the same mutations in the LREs known to abolish Lin28 binding and stimulation of translation also abrogate Drosha-dependent mRNA destabilization, and that this effect is independent of miRNAs, uncovering a previously unsuspected coupling between Drosha-dependent destabilization and Lin28-mediated regulation. Thus, Lin28-dependent stimulation of translation of target mRNAs may, in part, serve to compensate for their intrinsic instability, thereby ensuring optimal levels of expression of genes critical for cell viability, metabolism and pluripotency.

摘要

Lin28 在发育、干细胞维持、肿瘤发生和代谢中发挥重要作用。作为一种 RNA 结合蛋白,它主要阻断 let-7 家族 miRNA 的生物发生,同时促进涉及细胞生长、代谢和多能性的一组 mRNA 的翻译,可能通过识别 mRNA 内的不同序列和结构基序。在这里,我们表明,Lin28 响应元件 (LRE) 中的一个这样的基序,存在于 Lin28 mRNA 靶标中,也参与 Drosha 依赖性调节,并可能有助于其同源 mRNA 的不稳定性。我们进一步表明,已知在 LRE 中发生的突变,这些突变可消除 Lin28 结合并刺激翻译,也可消除 Drosha 依赖性 mRNA 不稳定性,并且这种效应不依赖于 miRNAs,揭示了 Drosha 依赖性不稳定性和 Lin28 介导的调节之间以前未被怀疑的偶联。因此,Lin28 依赖性靶 mRNA 翻译的刺激可能部分用于补偿其内在不稳定性,从而确保与细胞活力、代谢和多能性相关的关键基因的最佳表达水平。

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