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MicroRNA Directly Enhances Mitochondrial Translation during Muscle Differentiation

机译:MicroRNA在肌肉分化过程中直接增强线粒体翻译

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摘要

MicroRNAs are well known to mediate translational repression and mRNA degradation in the cytoplasm. Various microRNAs have also been detected in membrane- compartmentalized organelles, but the functional significance has remained elusive. Here, we report that miR-1, a microRNA specifically induced during myogenesis, efficiently enters the mitochondria where it unexpectedly stimulates, rather than represses, the translation of specific mitochondrial genome-encoded transcripts. We show that this positive effect requires specific miR:mRNA basepairing and Ago2, but not its functional partner GW182, which is excluded from the mitochondria. We provide evidence for the direct action of Ago2 in mitochondrial translation by crosslinking immunoprecipitation coupled with deep sequencing (CLIPseq), functional rescue with mitochondria-targeted Ago2, and selective inhibition of the microRNA machinery in the cytoplasm. These findings unveil a positive function of microRNA in mitochondrial translation and suggest a highly coordinated myogenic program via miR-1-mediated translational stimulation in the mitochondria and repression in the cytoplasm.
机译:众所周知,微小RNA介导细胞质中的翻译抑制和mRNA降解。在膜区隔的细胞器中也检测到了各种microRNA,但其功能意义仍然难以捉摸。在这里,我们报道了miR-1,一种在成肌过程中特异性诱导的microRNA,有效进入线粒体,意外地刺激而不是抑制特定线粒体基因组编码的转录本的翻译。我们表明,这种积极的影响需要特定的miR:mRNA碱基配对和Ago2,但不需要其功能伙伴GW182,而线粒体除外。我们提供的证据表明,Ago2在线粒体翻译中的直接作用是通过交联免疫沉淀结合深度测序(CLIPseq),以线粒体为靶点的Ago2进行功能性拯救以及对细胞质中microRNA机制的选择性抑制。这些发现揭示了microRNA在线粒体翻译中的积极作用,并暗示了通过miR-1介导的线粒体翻译刺激和细胞质阻遏作用的高度协调的成肌程序。

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