Modulation of pulmonary vascular smooth muscle cell phenotype in hypoxia: role of cGMP-dependent protein kinase and myocardin

doi:10.1152/ajplung.90295.2008

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Am J Physiol Lung Cell Mol Physiol 296: L780-L789, 2009. First published February 27, 2009; doi:10.1152/ajplung.90295.2008
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Modulation of pulmonary vascular smooth muscle cell phenotype in hypoxia: role of cGMP-dependent protein kinase and myocardin

Weilin Zhou,¹ Sewite Negash,¹ Jie Liu,¹ and J. Usha Raj²

¹Division of Neonatology, Harbor-UCLA Medical Center, Los Angeles Biomedical Research Institute at Harbor-UCLA, Torrance, California; and ²Department of Pediatrics, University of Illinois at Chicago, Chicago, Illinois

Submitted 1 May 2008 ; accepted in final form 9 February 2009

We have previously reported that in ovine fetal pulmonary venoussmooth muscle cells (FPVSMC), decreased expression of cGMP-dependentprotein kinase (PKG) by hypoxia could explain hypoxia-inducedSMC phenotype modulation. In this study, we investigated therole of myocardin, a possible downstream effector of PKG, inSMC phenotype modulation induced by 1 and 24 h of hypoxia. Hypoxiafor 1 h induced the phosphorylation of E-26-like protein 1 (Elk-1),indicating a quick activation of Elk-1 after hypoxia. Eitherhypoxia (1 h) or treatment with DT-3, a PKG inhibitor, increasedassociations of Elk-1 with myosin heavy chain (MHC) gene andserum response factor (SRF), which was paralleled by a decreasein association of myocardin with MHC gene and SRF. Exposureto hypoxia of FPVSMC for 24 h significantly decreased the promoteractivity of multiple SMC marker genes, downregulated proteinand mRNA expression of myocardin, and upregulated mRNA expressionof Elk-1, but had no significant effects on the phosphorylationof Elk-1. Inhibition of myocardin by siRNA transfection downregulatedthe expression of SMC marker proteins, while overexpressionof myocardin prevented the hypoxia-induced decrease in expressionof SMC marker proteins. Inhibition of PKG by siRNA transfectiondownregulated the expression of myocardin, but upregulated thatof Elk-1. Overexpression of PKG prevented hypoxia-induced effectson protein expression of myocardin and Elk-1. These data suggestthat PKG induces displacement of myocardin from SRF and upregulatesmyocardin expression, thus activating the SMC genes transcription.The inhibitory effects of hypoxia on PKG may explain hypoxia-inducedSMC phenotype modulation by decreasing the effects of PKG onmyocardin.

Elk-1

Address for reprint requests and other correspondence: W. Zhou, Division of Neonatology, Harbor-UCLA Medical Center, Los Angeles Biomedical Research Institute at Harbor-UCLA, 1124 West Carson St., Torrance, CA 90502 (e-mail: zhouweilin{at}yahoo.com)