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Publication : RBM4-MEF2C network constitutes a feed-forward circuit that facilitates the differentiation of brown adipocytes.

First Author  Lin JC Year  2015
Journal  RNA Biol Volume  12
Issue  2 Pages  208-20
PubMed ID  25826570 Mgi Jnum  J:320310
Mgi Id  MGI:6868890 Doi  10.1080/15476286.2015.1017213
Citation  Lin JC (2015) RBM4-MEF2C network constitutes a feed-forward circuit that facilitates the differentiation of brown adipocytes. RNA Biol 12(2):208-20
abstractText  Myocyte enhancer factor 2c (MEF2C) is the MADS-box type transcription factor involved in the differentiation of cardiac and skeletal muscle and synaptic formation. Alternatively spliced transcripts of the MEF2C gene were proven to encode isoforms which exert distinct functions in transcriptional regulation. During the differentiation of brown adipocytes, upregulated RBM4 enhanced skipping of the MEF2Cgamma region which functions as a transcriptional repressor. The presence of an overexpressed MEF2Cgamma- isoform in turn induced transcriptional activity of the RBM4 promoter, constituting a positive feedback circuit in differentiating brown adipocytes. The RBM4-MEF2Cgamma- network induced the expression of "myogenic" miR-1 to a greater extent than did PRDM17, BMP7 C/EBPbeta, or UCP1 transcripts in C3H10T1/2 cells. Overexpression of miR-1 independently exerted the same activity as RBM4 and the MEF2Cgamma- isoform of upregulating brown adipocyte-specific factors in C3H10T1/2 cells, which suggests a potential effect of miR-1 on brown adipocytes. These results indicated that the RBM4-MEF2C-miR-1 network constitutes a novel mechanism which programs the gene expression profile toward the development of brown adipocytes.
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