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Abstract

Objective: Smooth muscle cell (SMC) migration involves interactions with extracellular matrix (ECM) and is an important process in response to arterial wall injury. We investigated the expression and the functional role of vitronectin (VN) in the response after vascular injury. Methods: VN and αvβ3/β5 integrin expressions were investigated after balloon carotid injury of Sprague–Dawley rats. Adventitial delivery of blocking antibodies to VN, αvβ5 and β3 integrins were performed to assess their roles in neointima formation. In vitro, migration assays were carried out on human SMC. Results: Immunohistochemistry and in situ hybridization for VN showed an upregulation of VN during the early time points of intima formation. αvβ3/β5 integrins expression correlated with VN expression. After 7 days, blocking antibodies to VN, αvβ5 and β3 induced a significant decrease on intimal area associated with a decrease in intimal cell counts. A slight decrease in intimal cell proliferation without any effect on apoptosis was observed after VN blockade. In vitro, migrating SMC strongly expressed VN after injury and neutralizing anti-VN antibody inhibited SMC migration. Blocking experiment with anti-αvβ5 and -αvβ3 integrin antibodies showed that not only VN–αvβ3 but also VN–αvβ5 interactions are required for SMC migration. Conclusion: This study characterizes the VN–ECM interaction in SMC and supports the role of VN in mediating SMC migration and neointimal formation in response to injury.

Cell culture/isolation, Extracellular matrix, Gene expression, Restenosis, Smooth muscle
ECM, extracellular matrix, MMP, matrix metalloproteinase, PAI-1, plasminogen activator inhibitor-1, SMC, smooth muscle cell, tPA, tissue-plasminogen activator, uPA, urokinase, VN, vitronectin
Copyright © 2002, European Society of Cardiology
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Original Article
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