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Publication : CHAMP, a novel cardiac-specific helicase regulated by MEF2C.

First Author  Liu ZP Year  2001
Journal  Dev Biol Volume  234
Issue  2 Pages  497-509
PubMed ID  11397016 Mgi Jnum  J:69957
Mgi Id  MGI:2135830 Doi  10.1006/dbio.2001.0277
Citation  Liu ZP, et al. (2001) CHAMP, a novel cardiac-specific helicase regulated by MEF2C. Dev Biol 234(2):497-509
abstractText  MEF2C is a MADS-box transcription factor required for cardiac myogenesis and morphogenesis. In MEF2C mutant mouse embryos, heart development arrests at the looping stage (embryonic day 9.0), the future right ventricular chamber fails to form, and cardiomyocyte differentiation is disrupted. To identify genes regulated by MEF2C in the developing heart, we performed differential array analysis coupled with subtractive cloning using RNA from heart tubes of wild-type and MEF2C-null embryos. Here, we describe a novel MEF2C-dependent gene that encodes a cardiac-restricted protein, called CHAMP (cardiac helicase activated by MEF2 protein), that contains seven conserved motifs characteristic of helicases involved in RNA processing, DNA replication, and transcription. During mouse embryogenesis, CHAMP expression commences in the linear heart tube at embryonic day 8.0, shortly after initiation of MEF2C expression in the cardiogenic region. Thereafter, CHAMP is expressed specifically in embryonic and postnatal cardiomyocytes. At the trabeculation stage of heart development, CHAMP expression is highest in the trabecular region in which cardiomyocytes have exited the cell cycle and is lowest in the proliferative compact zone. These findings suggest that CHAMP acts downstream of MEF2C in a cardiac-specific regulatory pathway for RNA processing and/or transcriptional control. Copyright 2001 Academic Press.
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