Biomechanical regulation of hedgehog signaling in vascular smooth muscle cells in vitro and in vivo

doi:10.1152/ajpcell.00337.2005

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Am J Physiol Cell Physiol 292: C488-C496, 2007. First published August 30, 2006; doi:10.1152/ajpcell.00337.2005
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VASCULAR BIOLOGY

Biomechanical regulation of hedgehog signaling in vascular smooth muscle cells in vitro and in vivo

David Morrow,¹ Catherine Sweeney,¹ Yvonne A. Birney,¹ Shaunta Guha,¹ Nora Collins, Philip M. Cummins,¹ Ronan Murphy,¹ Dermot Walls,² Eileen M. Redmond,³ and Paul A. Cahill¹

¹Vascular Health Research Centre, Faculty of Science and Health, and ²School of Biotechnology and the National Centre for Sensor Research, Dublin City University, Dublin, Ireland; and ³Department of Surgery, University of Rochester Medical Center, Rochester, New York

Submitted 8 July 2005 ; accepted in final form 23 August 2006

Hedgehog (Hh) signaling has recently been shown to be both responsiveto mechanical loading in vitro and to control vascular developmentin vivo. We investigated the role of cyclic strain and pulsatileflow in modulating Hh signaling and growth of adult rat vascularsmooth muscle cells (SMC) in culture. Exposure of SMC to definedequibiaxial cyclic strain (0% and 10% stretch, 60 cycles/min,for 24 h) significantly decreased sonic hedgehog (Shh) and patched1 (Ptc1) expression while concurrently inhibiting Gli₂-dependentpromoter activity and mRNA expression, respectively. Cyclicstrain significantly decreased SMC proliferation (cell countsand proliferating cell nuclear antigen expression) concomitantwith a marked increase in SMC apoptosis (fluorescence-activatedcell sorter analysis, acridine orange staining of apoptoticnuclei and Bax/Bcl-x_L ratio). These strain-induced changes inproliferation and apoptosis were significantly attenuated followingaddition of either recombinant Shh (3.5 µg/ml) or overexpressionof the Notch 3 intracellular domain (Notch IC). Further studiesusing a perfused transcapillary culture system demonstrateda significant decrease in Hh signaling in SMC following exposureof cells to increased pulsatile flow concomitant with a decreasein proliferation and an increase in apoptosis. Finally, thepulsatile flow-induced decreases in Hh signaling were validatedin vivo following flow-induced rat carotid arterial remodelingafter 28 days. These data suggest that Hh expression is diminishedby biomechanical stimulation in vitro and in vivo and thus mayplay a fundamental role in arterial remodeling and atherogenesisin vivo.

cyclic strain; apoptosis; proliferation

Address for reprint requests and other correspondence: P. A. Cahill, Faculty of Science and Health, Vascular Health Research Centre, Glasnevin, Dublin 9, Ireland (e-mail: paul.cahill{at}dcu.ie)

This article has been cited by other articles:

D. Morrow, J. P. Cullen, W. Liu, S. Guha, C. Sweeney, Y. A. Birney, N. Collins, D. Walls, E. M. Redmond, and P. A. Cahill
Sonic Hedgehog Induces Notch Target Gene Expression in Vascular Smooth Muscle Cells via VEGF-A
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