| Literature DB >> 29606596 |
Stas Wüst1, Stefan Dröse2, Juliana Heidler3, Ilka Wittig3, Ina Klockner1, Andras Franko4, Erik Bonke2, Stefan Günther1, Ulrich Gärtner5, Thomas Boettger6, Thomas Braun7.
Abstract
Muscle stem cells undergo a dramatic metabolic switch to oxidative phosphorylation during differentiation, which is achieved by massively increased mitochondrial activity. Since expression of the muscle-specific miR-1/133a gene cluster correlates with increased mitochondrial activity during muscle stem cell (MuSC) differentiation, we examined the potential role of miR-1/133a in metabolic maturation of skeletal muscles in mice. We found that miR-1/133a downregulate Mef2A in differentiated myocytes, thereby suppressing the Dlk1-Dio3 gene cluster, which encodes multiple microRNAs inhibiting expression of mitochondrial genes. Loss of miR-1/133a in skeletal muscles or increased Mef2A expression causes continuous high-level expression of the Dlk1-Dio3 gene cluster, compromising mitochondrial function. Failure to terminate the stem cell-like metabolic program characterized by high-level Dlk1-Dio3 gene cluster expression initiates profound changes in muscle physiology, essentially abrogating endurance running. Our results suggest a major role of miR-1/133a in metabolic maturation of skeletal muscles but exclude major functions in muscle development and MuSC maintenance.Entities:
Keywords: Dlk1-Dio3; Mef2A; miR-1; miR-133a; microRNA; skeletal muscle metabolism; skeletal muscle mitochondria; skeletal muscle stem cells
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Year: 2018 PMID: 29606596 DOI: 10.1016/j.cmet.2018.02.022
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287