Bortezomib protects from varicose‐like venous remodeling

Despite the high prevalence of venous diseases that are associated with and based on the structural reorganization of the venous vessel wall, not much is known about their mechanistic causes. In this context, we demonstrated that the quantity of myocardin, a transcriptional regulator of the contract...

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Veröffentlicht in:	The FASEB journal 2014-08, Vol.28 (8), p.3518-3527
Hauptverfasser:	Pfisterer, Larissa, Meyer, Ralph, Feldner, Anja, Drews, Oliver, Hecker, Markus, Korff, Thomas
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Sprache:	eng
Schlagworte:	Animals Animals, Outbred Strains Boronic Acids - pharmacology Boronic Acids - therapeutic use Bortezomib Cell Division - drug effects Cell Movement Cells, Cultured Collagen Disease Models, Animal Drug Evaluation, Preclinical Humans Mice Muscle, Smooth, Vascular - pathology myocardin Myocytes, Smooth Muscle - cytology Myocytes, Smooth Muscle - drug effects Myocytes, Smooth Muscle - metabolism Nuclear Proteins - metabolism Protease Inhibitors - pharmacology Protease Inhibitors - therapeutic use proteasome Proteasome Endopeptidase Complex - physiology Proteolysis Pyrazines - pharmacology Pyrazines - therapeutic use Spheroids, Cellular Trans-Activators - metabolism varicose veins Varicose Veins - drug therapy Varicose Veins - enzymology Varicose Veins - pathology venous smooth muscle cell phenotype
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creator	Pfisterer, Larissa Meyer, Ralph Feldner, Anja Drews, Oliver Hecker, Markus Korff, Thomas
description	Despite the high prevalence of venous diseases that are associated with and based on the structural reorganization of the venous vessel wall, not much is known about their mechanistic causes. In this context, we demonstrated that the quantity of myocardin, a transcriptional regulator of the contractile and quiescent smooth muscle cell phenotype, was diminished in proliferating synthetic venous smooth muscle cells (VSMCs) of human and mouse varicose veins by 51 and 60%, respectively. On the basis of the relevance of proteasomal activity for such phenotypic changes, we hypothesized that the observed VSMC activation is attenuated by the proteasome inhibitor bortezomib. This drug fully abolished VSMC proliferation and loss of myocardin in perfused mouse veins and blocked VSMC invasion in collagen gels by almost 80%. In line with this, topical transdermal treatment with bortezomib diminished VSMC proliferation by 80%, rescued 90% of VSMC myocardin abundance, and inhibited varicose‐like venous remodeling by 67 to 72% in a mouse model. Collectively, our data indicate that the proteasome plays a pivotal role in VSMC phenotype changes during venous remodeling processes. Its inhibition protects from varicose‐like vein remodeling in mice and may thus serve as a putative therapeutic strategy to treat human varicose veins.—Pfisterer, L., Meyer, R., Feldner, A., Drews, O., Hecker, M., Korff, T. Bortezomib protects from varicose‐like venous remodeling. FASEB J. 28, 3518–3527 (2014). www.fasebj.org
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In this context, we demonstrated that the quantity of myocardin, a transcriptional regulator of the contractile and quiescent smooth muscle cell phenotype, was diminished in proliferating synthetic venous smooth muscle cells (VSMCs) of human and mouse varicose veins by 51 and 60%, respectively. On the basis of the relevance of proteasomal activity for such phenotypic changes, we hypothesized that the observed VSMC activation is attenuated by the proteasome inhibitor bortezomib. This drug fully abolished VSMC proliferation and loss of myocardin in perfused mouse veins and blocked VSMC invasion in collagen gels by almost 80%. In line with this, topical transdermal treatment with bortezomib diminished VSMC proliferation by 80%, rescued 90% of VSMC myocardin abundance, and inhibited varicose‐like venous remodeling by 67 to 72% in a mouse model. Collectively, our data indicate that the proteasome plays a pivotal role in VSMC phenotype changes during venous remodeling processes. Its inhibition protects from varicose‐like vein remodeling in mice and may thus serve as a putative therapeutic strategy to treat human varicose veins.—Pfisterer, L., Meyer, R., Feldner, A., Drews, O., Hecker, M., Korff, T. Bortezomib protects from varicose‐like venous remodeling. 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In this context, we demonstrated that the quantity of myocardin, a transcriptional regulator of the contractile and quiescent smooth muscle cell phenotype, was diminished in proliferating synthetic venous smooth muscle cells (VSMCs) of human and mouse varicose veins by 51 and 60%, respectively. On the basis of the relevance of proteasomal activity for such phenotypic changes, we hypothesized that the observed VSMC activation is attenuated by the proteasome inhibitor bortezomib. This drug fully abolished VSMC proliferation and loss of myocardin in perfused mouse veins and blocked VSMC invasion in collagen gels by almost 80%. In line with this, topical transdermal treatment with bortezomib diminished VSMC proliferation by 80%, rescued 90% of VSMC myocardin abundance, and inhibited varicose‐like venous remodeling by 67 to 72% in a mouse model. Collectively, our data indicate that the proteasome plays a pivotal role in VSMC phenotype changes during venous remodeling processes. Its inhibition protects from varicose‐like vein remodeling in mice and may thus serve as a putative therapeutic strategy to treat human varicose veins.—Pfisterer, L., Meyer, R., Feldner, A., Drews, O., Hecker, M., Korff, T. Bortezomib protects from varicose‐like venous remodeling. 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Its inhibition protects from varicose‐like vein remodeling in mice and may thus serve as a putative therapeutic strategy to treat human varicose veins.—Pfisterer, L., Meyer, R., Feldner, A., Drews, O., Hecker, M., Korff, T. Bortezomib protects from varicose‐like venous remodeling. FASEB J. 28, 3518–3527 (2014). www.fasebj.org</abstract><cop>United States</cop><pub>The Federation of American Societies for Experimental Biology</pub><pmid>24769668</pmid><doi>10.1096/fj.14-250464</doi><tpages>10</tpages><oa>free_for_read</oa></addata></record>
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subjects	Animals Animals, Outbred Strains Boronic Acids - pharmacology Boronic Acids - therapeutic use Bortezomib Cell Division - drug effects Cell Movement Cells, Cultured Collagen Disease Models, Animal Drug Evaluation, Preclinical Humans Mice Muscle, Smooth, Vascular - pathology myocardin Myocytes, Smooth Muscle - cytology Myocytes, Smooth Muscle - drug effects Myocytes, Smooth Muscle - metabolism Nuclear Proteins - metabolism Protease Inhibitors - pharmacology Protease Inhibitors - therapeutic use proteasome Proteasome Endopeptidase Complex - physiology Proteolysis Pyrazines - pharmacology Pyrazines - therapeutic use Spheroids, Cellular Trans-Activators - metabolism varicose veins Varicose Veins - drug therapy Varicose Veins - enzymology Varicose Veins - pathology venous smooth muscle cell phenotype
title	Bortezomib protects from varicose‐like venous remodeling
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