In Vitro Evidence Suggests That MiR-133a-mediated Regulation of Uncoupling Protein 2 (UCP2) is an Indispensable Step in Myogenic Differentiation

Overview

Journal J Biol Chem

Specialty Biochemistry

Date 2008 Dec 17

PMID 19073597

Citations 54

Authors

Xi Chen

Kehui Wang

Jiangning Chen

Jigang Guo

Yuan Yin

Xing Cai

Xing Guo

Guoqiang Wang

Rong Yang

Lingyun Zhu

Yan Zhang

Jin Wang

Yang Xiang

Chunyue Weng

Ke Zen

Junfeng Zhang

Chen-Yu Zhang

Affiliations

Soon will be listed here.

Abstract

UCP2 and UCP3, two novel uncoupling proteins, are important regulators of energy expenditure and thermogenesis in various organisms. The striking disparity between UCP2 mRNA and protein levels in muscle tissues prompted initial speculation that microRNAs are implicated in the regulatory pathway of UCP2. We found, for the first time, that the repression of UCP2 expression in cardiac and skeletal muscle resulted from its targeting by a muscle-specific microRNA, miR-133a. Moreover, our findings illustrate a novel function of UCP2 as a brake for muscle development. We also show that MyoD can remove the braking role of UCP2 via direct up-regulation of miR-133a during myogenic differentiation. Taken together, our current work delineates a novel regulatory network employing MyoD, microRNA, and uncoupling proteins to fine-tune the balance between muscle differentiation and proliferation during myogenesis.

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