The G534E polymorphism of the gene encoding the factor VII–activating protease is associated with cardiovascular risk due to increased neointima formation

The G534E polymorphism (Marburg I [MI]) of factor VII–activating protease (FSAP) is associated with carotid stenosis and cardiovascular disease. We have previously demonstrated that FSAP is present in atherosclerotic plaques and it is a potent inhibitor of vascular smooth muscle proliferation and mi...

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Autores principales: Sedding, Daniel, Daniel, Jan-Marcus, Muhl, Lars, Hersemeyer, Karin, Brunsch, Hannes, Kemkes-Matthes, Bettina, Braun-Dullaeus, Ruediger C., Tillmanns, Harald, Weimer, Thomas, Preissner, Klaus T., Kanse, Sandip M.
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2006
Materias:
Brief Definitive Reports
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2118185/
https://www.ncbi.nlm.nih.gov/pubmed/17145954
http://dx.doi.org/10.1084/jem.20052546
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author Sedding, Daniel
Daniel, Jan-Marcus
Muhl, Lars
Hersemeyer, Karin
Brunsch, Hannes
Kemkes-Matthes, Bettina
Braun-Dullaeus, Ruediger C.
Tillmanns, Harald
Weimer, Thomas
Preissner, Klaus T.
Kanse, Sandip M.
author_facet Sedding, Daniel
Daniel, Jan-Marcus
Muhl, Lars
Hersemeyer, Karin
Brunsch, Hannes
Kemkes-Matthes, Bettina
Braun-Dullaeus, Ruediger C.
Tillmanns, Harald
Weimer, Thomas
Preissner, Klaus T.
Kanse, Sandip M.
author_sort Sedding, Daniel
collection PubMed
description The G534E polymorphism (Marburg I [MI]) of factor VII–activating protease (FSAP) is associated with carotid stenosis and cardiovascular disease. We have previously demonstrated that FSAP is present in atherosclerotic plaques and it is a potent inhibitor of vascular smooth muscle proliferation and migration in vitro. The effect of wild-type (WT)- and MI-FSAP on neointima formation in the mouse femoral artery after wire-induced injury was investigated. Local application of WT-FSAP led to a 70% reduction in the neointima formation, and this effect was dependent on the protease activity of FSAP. MI-FSAP did not inhibit neointima formation in vivo. This is due to a reduced proteolytic activity of MI-FSAP, compared to WT-FSAP, toward platelet-derived growth factor BB, a key mediator of neointima development. The inability of MI-FSAP to inhibit vascular smooth muscle accumulation explains the observed linkage between the MI-polymorphism and increased cardiovascular risk. Hence, FSAP has a protective function in the vasculature, and analysis of MI polymorphism is likely to be clinically relevant in restenosis.
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spelling pubmed-21181852007-12-13 The G534E polymorphism of the gene encoding the factor VII–activating protease is associated with cardiovascular risk due to increased neointima formation Sedding, Daniel Daniel, Jan-Marcus Muhl, Lars Hersemeyer, Karin Brunsch, Hannes Kemkes-Matthes, Bettina Braun-Dullaeus, Ruediger C. Tillmanns, Harald Weimer, Thomas Preissner, Klaus T. Kanse, Sandip M. J Exp Med Brief Definitive Reports The G534E polymorphism (Marburg I [MI]) of factor VII–activating protease (FSAP) is associated with carotid stenosis and cardiovascular disease. We have previously demonstrated that FSAP is present in atherosclerotic plaques and it is a potent inhibitor of vascular smooth muscle proliferation and migration in vitro. The effect of wild-type (WT)- and MI-FSAP on neointima formation in the mouse femoral artery after wire-induced injury was investigated. Local application of WT-FSAP led to a 70% reduction in the neointima formation, and this effect was dependent on the protease activity of FSAP. MI-FSAP did not inhibit neointima formation in vivo. This is due to a reduced proteolytic activity of MI-FSAP, compared to WT-FSAP, toward platelet-derived growth factor BB, a key mediator of neointima development. The inability of MI-FSAP to inhibit vascular smooth muscle accumulation explains the observed linkage between the MI-polymorphism and increased cardiovascular risk. Hence, FSAP has a protective function in the vasculature, and analysis of MI polymorphism is likely to be clinically relevant in restenosis. The Rockefeller University Press 2006-12-25 /pmc/articles/PMC2118185/ /pubmed/17145954 http://dx.doi.org/10.1084/jem.20052546 Text en Copyright © 2006, The Rockefeller University Press This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Brief Definitive Reports
Sedding, Daniel
Daniel, Jan-Marcus
Muhl, Lars
Hersemeyer, Karin
Brunsch, Hannes
Kemkes-Matthes, Bettina
Braun-Dullaeus, Ruediger C.
Tillmanns, Harald
Weimer, Thomas
Preissner, Klaus T.
Kanse, Sandip M.
The G534E polymorphism of the gene encoding the factor VII–activating protease is associated with cardiovascular risk due to increased neointima formation
title The G534E polymorphism of the gene encoding the factor VII–activating protease is associated with cardiovascular risk due to increased neointima formation
title_full The G534E polymorphism of the gene encoding the factor VII–activating protease is associated with cardiovascular risk due to increased neointima formation
title_fullStr The G534E polymorphism of the gene encoding the factor VII–activating protease is associated with cardiovascular risk due to increased neointima formation
title_full_unstemmed The G534E polymorphism of the gene encoding the factor VII–activating protease is associated with cardiovascular risk due to increased neointima formation
title_short The G534E polymorphism of the gene encoding the factor VII–activating protease is associated with cardiovascular risk due to increased neointima formation
title_sort g534e polymorphism of the gene encoding the factor vii–activating protease is associated with cardiovascular risk due to increased neointima formation
topic Brief Definitive Reports
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2118185/
https://www.ncbi.nlm.nih.gov/pubmed/17145954
http://dx.doi.org/10.1084/jem.20052546
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