| Literature DB >> 25887157 |
Xiaoping Peng1, Xiaopeng Shen2, Xuanying Chen1, Rui Liang2, Alon R Azares3, Yu Liu4.
Abstract
Myotonic dystrophy is a neuromuscular disease of RNA toxicity. The disease gene DMPK harbors expanded CTG trinucleotide repeats on its 3'-UTR. The transcripts of this mutant DMPK led to misregulation of RNA-binding proteins including MBNL1 and Celf1. In myoblasts, CUG-expansion impaired terminal differentiation. In this study, we formally tested how the abundance of Celf1 regulates normal myocyte differentiation, and how Celf1 expression level mediates CUG-expansion RNA toxicity-triggered impairment of myocyte differentiation. As the results, overexpression of Celf1 largely recapitulated the defects of myocytes with CUG-expansion, by increasing myocyte cycling. Knockdown of endogenous Celf1 level led to precocious myotube formation, supporting a negative connection between Celf1 abundance and myocyte terminal differentiation. Finally, knockdown of Celf1 in myocyte with CUG-expansion led to partial rescue, by promoting cell cycle exit. Our results suggest that Celf1 plays a distinctive and negative role in terminal myocyte differentiation, which partially contribute to DM1 RNA toxicity. Targeting Celf1 may be a valid strategy in correcting DM1 muscle phenotypes, especially for congenital cases.Entities:
Keywords: CUGBP1; Celf1; Differentiation; Myoblast; Myotonic dystrophy
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Year: 2015 PMID: 25887157 DOI: 10.1016/j.bbadis.2015.04.010
Source DB: PubMed Journal: Biochim Biophys Acta ISSN: 0006-3002