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The H19 long noncoding RNA gives rise to microRNAs miR-675-3p and miR-675-5p to promote skeletal muscle differentiation and regeneration

机译:H19长非编码RNA产生了miR-675-3p和miR-675-5p以促进骨骼肌的分化和再生

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摘要

Regulated expression of the H19 long noncoding RNA gene has been well characterized as a paradigm for genomic imprinting, but the H19 RNA's biological function remains largely unclear. H19 is abundantly expressed maternally in embryonic tissues but is strongly repressed after birth, and significant transcription persists only in skeletal muscle. Thus, we examined the role of the H19 RNA in skeletal muscle differentiation and regeneration. Knockdown of H19 RNA in myoblast cells and H19 knockout mouse satellite cells decreases differentiation. H19 exon1 encodes two conserved microRNAs, miR-675-3p and miR-675-5p, both of which are induced during skeletal muscle differentiation. The inhibition of myogenesis by H19 depletion during myoblast differentiation is rescued by exogenous expression of miR-675-3p and miR-675-5p. H19-deficient mice display abnormal skeletal muscle regeneration after injury, which is rectified by reintroduction of miR-675-3p and miR-675-5p. miR-675-3p and miR-675-5p function by directly targeting and down-regulating the anti-differentiation Smad transcription factors critical for the bone morphogenetic protein (BMP) pathway and the DNA replication initiation factor Cdc6. Therefore, the H19 long noncoding RNA has a critical trans-regulatory function in skeletal muscle differentiation and regeneration that is mediated by the microRNAs encoded within H19.
机译:H19长非编码RNA基因的调控表达已被很好地描述为基因组印迹的范例,但H19 RNA的生物学功能仍不清楚。 H19在孕产妇中在胚胎组织中大量表达,但在出生后会受到强烈抑制,并且仅在骨骼肌中存在明显的转录。因此,我们检查了H19 RNA在骨骼肌分化和再生中的作用。敲除成肌细胞和H19敲除小鼠卫星细胞中的H19 RNA会降低分化。 H19 exon1编码两个保守的microRNA,即miR-675-3p和miR-675-5p,它们均在骨骼肌分化过程中被诱导。通过miR-675-3p和miR-675-5p的外源表达挽救了成肌细胞分化期间H19耗竭对肌发生的抑制作用。 H19缺陷小鼠在受伤后显示异常的骨骼肌再生,这可以通过重新引入miR-675-3p和miR-675-5p来纠正。 miR-675-3p和miR-675-5p通过直接靶向和下调对骨形态发生蛋白(BMP)途径和DNA复制起始因子Cdc6至关重要的抗分化Smad转录因子而起作用。因此,H19长的非编码RNA在骨骼肌的分化和再生中具有关键的反式调节功能,该功能由H19内编码的微小RNA介导。

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