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Interaction of<i>OIP5-AS1</i>with<i>MEF2C</i>mRNA promotes myogenic gene expression

Jen‐Hao Yang, Ming‐Wen Chang, Poonam R. Pandey, Dimitrios Tsitsipatis, Xiaoling Yang, Jennifer L. Martindale, Rachel Munk, Supriyo De, Kotb Abdelmohsen, Myriam Gorospe

2020Nucleic Acids Research40 citationsDOIOpen Access PDF

Abstract

Long noncoding (lnc)RNAs potently regulate gene expression programs in physiology and disease. Here, we describe a key function for lncRNA OIP5-AS1 in myogenesis, the process whereby myoblasts differentiate into myotubes during muscle development and muscle regeneration after injury. In human myoblasts, OIP5-AS1 levels increased robustly early in myogenesis, and its loss attenuated myogenic differentiation and potently reduced the levels of the myogenic transcription factor MEF2C. This effect relied upon the partial complementarity of OIP5-AS1 with MEF2C mRNA and the presence of HuR, an RNA-binding protein (RBP) with affinity for both transcripts. Remarkably, HuR binding to MEF2C mRNA, which stabilized MEF2C mRNA and increased MEF2C abundance, was lost after OIP5-AS1 silencing, suggesting that OIP5-AS1 might serve as a scaffold to enhance HuR binding to MEF2C mRNA, in turn increasing MEF2C production. These results highlight a mechanism whereby a lncRNA promotes myogenesis by enhancing the interaction of an RBP and a myogenic mRNA.

Topics & Concepts

MyogenesisMEF2CBiologyMessenger RNAGene expressionGene silencingCell biologyMyocyteTranscription factorRegulation of gene expressionMolecular biologyGeneGeneticsCancer-related molecular mechanisms researchRNA Research and SplicingPlant and Fungal Interactions Research
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