{alpha}8 Integrin expression is required for maintenance of the smooth muscle cell differentiated phenotype

doi:10.1016/j.cardiores.2006.03.003

Cardiovascular Research 2006 71(1):170-178; doi:10.1016/j.cardiores.2006.03.003

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${alpha}$ 8 Integrin expression is required for maintenance of the smooth muscle cell differentiated phenotype

Ramin Zargham and Gaétan Thibault^*

Institut de recherches cliniques de Montréal, Université de Montréal and Department of Experimental Medicine, McGill University, 110, avenue des Pins ouest, Montréal, Québec, Canada H2W 1R7

^* Corresponding author. Tel.: +1 514 987 5613; fax: +1 514 987 5585. Email address: thibaug{at}ircm.qc.ca

Objective Vascular smooth muscle cell (VSMC) de-differentiationis a prerequisite for migration from the tunica media to theintima after vascular injury. Integrin cell adhesion moleculesparticipate in VSMC phenotype modulation. ${alpha}$ 8β1 Integrinis a differentiation marker of VSMCs and its knockdown heightensmigration. In the present study, we examined whether or not ${alpha}$ 8 integrin is required for the maintenance of VSMC differentiatedphenotype.

Methods ${alpha}$ 8 Integrin in rat VSMC was knocked down by short interferenceRNA (siRNA) targeting ${alpha}$ 8 integrin in comparison to a non-silencingsiRNA. Cytoskeletal and morphological changes in VSMC were examinedby immunofluorescence staining. The expression of phenotype-dependentmarkers was analyzed by immunoblotting.

Results ${alpha}$ 8 Integrin gene silencing evoked drastic changes incharacteristics of the VSMC differentiated phenotype, includingVSMC morphology, actin fibre organization, focal adhesion assemblyand the expression of phenotype-dependent markers in favor ofde-differentiation. Then, we investigated whether or not phenotypemodulation induced by ${alpha}$ 8 integrin gene silencing could be reversedby an inducer of VSMC differentiation. Transforming growth factor-β(TGF-β) failed to upregulate smooth muscle-myosin heavychain as well as the assembly of parallel actin fibres in VSMCstransfected by siRNA- ${alpha}$ 8. In addition, TGF-β-induced vinculinlocalization at the tip of the cells was impaired by ${alpha}$ 8 integringene silencing.

Conclusion These data suggest that ${alpha}$ 8 integrin expression isrequired for maintenance of the VSMC differentiated phenotype,a state that is crucial for non-motile VSMCs.

KEYWORDS Angioplasty; Atherosclerosis; Cell differentiation; Cytoskeleton and smooth muscle

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