Developmental stage-specific regulation of atrial natriuretic factor gene transcription in cardiac cells.

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Mol Cell Biol. 1994 January; 14(1): 777-790

Developmental stage-specific regulation of atrial natriuretic factor gene transcription in cardiac cells.

S Argentin, A Ardati, S Tremblay, I Lihrmann, L Robitaille, J Drouin and M Nemer

Institut de recherches cliniques de Montréal, Université de Montréal, Québec, Canada.

ABSTRACT

Cardiac myocytes undergo a major genetic switch within the firstweek of postnatal development, when cell division ceases terminallyand many cardiac genes are either activated or silenced. Wehave developed stage-specific cardiocyte cultures to analyzetranscriptional control of the rat atrial natriuretic factor(ANF) gene to identify the mechanisms underlying tissue-specificand developmental regulation of this gene in the heart. Thefirst 700 bp of ANF flanking sequences was sufficient for cardiacmuscle- and stage-specific expression in both atrial and ventricularmyocytes, and a cardiac muscle-specific enhancer was localizedbetween -136 and -700 bp. Deletion of this enhancer markedlyreduced promoter activity in cardiac myocytes and derepressedANF promoter activity in nonexpressing cells. Two distinct domainsof the enhancer appeared to contribute differentially to cardiacspecificity depending on the differentiation stage of the myocytes.DNase I footprinting of the enhancer domain active in differentiatedcells revealed four putative regulatory elements including anA+T-rich region and a CArG element. Deletion mutagenesis andpromoter reconstitution assays revealed an important role forthe CArG-containing element exclusively in cardiac cells, whereits activity was switched on in differentiated myocytes. Transcriptionalactivity of the ANF-CArG box correlated with the presence ofa cardiac- and stage-specific DNA-binding complex which wasnot recognized by the c-fos serum response element. Thus, theuse of this in vitro model system representing stage-specificcardiac development unraveled the presence of different regulatorymechanisms for transcription of the ANF gene during cardiacdifferentiation and may be useful for studying the regulatorypathways of other genes that undergo switching during cardiacmyogenesis.

Mol Cell Biol. 1994 January; 14(1): 777-790

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