A hormone-encoding gene identifies a pathway for cardiac but not skeletal muscle gene transcription.

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Mol Cell Biol. 1994 May; 14(5): 3115-3129

A hormone-encoding gene identifies a pathway for cardiac but not skeletal muscle gene transcription.

C Grépin, L Dagnino, L Robitaille, L Haberstroh, T Antakly and M Nemer

Laboratoire de Développement et Différenciation Cardiaques, Institut de Recherches Cliniques de Montréal, Québec, Canada.

ABSTRACT

In contrast to skeletal muscle, the mechanisms responsible foractivation and maintenance of tissue-specific transcriptionin cardiac muscle remain poorly understood. A family of hormone-encodinggenes is expressed in a highly specific manner in cardiac butnot skeletal myocytes. This includes the A- and B-type natriureticpeptide (ANP and BNP) genes, which encode peptide hormones withcrucial roles in the regulation of blood volume and pressure.Since these genes are markers of cardiac cells, we have usedthem to probe the mechanisms for cardiac muscle-specific transcription.Cloning and functional analysis of the rat BNP upstream sequencesrevealed unexpected structural resemblance to erythroid butnot to muscle-specific promoters and enhancers, including arequirement for regulatory elements containing GATA motifs.A cDNA clone corresponding to a member of the GATA family oftranscription factors was isolated from a cardiomyocyte cDNAlibrary. Transcription of this GATA gene is restricted mostlyto the heart and is undetectable in skeletal muscle. Withinthe heart, GATA transcripts are localized in ANP- and BNP-expressingmyocytes, and forced expression of the GATA protein in heterologouscells markedly activates transcription from the natural cardiacmuscle-specific ANP and BNP promoters. This GATA-dependent pathwaydefines the first mechanism for cardiac muscle-specific transcription.Moreover, the present findings reveal striking similaritiesbetween the mechanisms controlling gene expression in hematopoieticand cardiac cells and may have important implications for studiesof cardiogenesis.

Mol Cell Biol. 1994 May; 14(5): 3115-3129

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