Contribution of serum response factor and myocardin to transcriptional regulation of smoothelins

doi:10.1016/j.cardiores.2005.12.018

Cardiovascular Research 2006 70(1):136-145; doi:10.1016/j.cardiores.2005.12.018

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Contribution of serum response factor and myocardin to transcriptional regulation of smoothelins

Sander S.M. Rensen^a, Petra M.G. Niessen^a, Xiaochun Long^c, Pieter A. Doevendans^b, Joseph M. Miano^c and Guillaume J.J.M. van Eys^a^,*

^aDepartment of Genetics and Cell Biology, Cardiovascular Research Institute Maastricht, University of Maastricht, Maastricht, The Netherlands
^bDepartment of Cardiology, Heart Lung Center Utrecht, Utrecht, The Netherlands and Interuniversity Cardiology Institute, Utrecht, The Netherlands
^cCardiovascular Research Institute, University of Rochester School of Medicine, Rochester, NY, United States

^* Corresponding author. University of Maastricht, Department of Genetics and Cell Biology, Universiteitssingel 50, PO Box 616, 6200 MD Maastricht, The Netherlands. Tel.: +31 43 3881355; fax: +31 43 3884149. Email address: g.vaneys{at}gen.unimaas.nl

Objective Smoothelin-A and -B isoforms are highly restrictedto contractile smooth muscle cells (SMCs). Serum response factor(SRF) and myocardin are essential for contractile SMC differentiation.We evaluated the contribution of SRF/myocardin to transcriptionalregulation of smoothelins.

Methods Rat vascular SMCs were transfected with smoothelin-Aand smoothelin-B promoter reporter constructs and promoter activitywas analyzed. The effects of mutations in the smoothelin-A promoterCArG-boxes and co-transfections with a myocardin expressionplasmid were assessed. Electrophoretic mobility shift assaysand chromatin immunoprecipitations were performed to investigateSRF-binding to the smoothelin-A CArG-boxes.

Results Smoothelin promoter activity was detected in vascularSMCs. Comparative sequence analysis revealed two conserved CArGelements in the smoothelin-A promoter that bind SRF as shownby chromatin immunoprecipitation. The proximal CArG-near boundSRF stronger than CArG-far in gel shift assays. Mutagenesisstudies also indicated that CArG-near is more important thanCArG-far in regulating smoothelin-A promoter activity. Myocardinaugmented smoothelin-A promoter activity 2.5-fold in a CArG-near-dependentmanner. In contrast, myocardin had little effect on the smoothelin-Bpromoter.

Conclusion Smoothelin-A expression is controlled by an intragenicpromoter whose activity is, in part, dependent on two CArG boxesthat bind SRF. Our data show a role for SRF/myocardin in regulatingsmoothelin-A whereas the higher smoothelin-B expression appearsto be SRF/myocardin-independent.

KEYWORDS Smoothelins; Myocardin; Serum response factor; Smooth muscle cell differentiation; Gene expression

Time for primary review 23 days

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