Gene Therapy With the Angiogenic Cytokine Secretoneurin Induces Therapeutic Angiogenesis by a Nitric Oxide-Dependent Mechanism

doi:10.1161/CIRCRESAHA.109.199513

Circulation Research. 2009
Published online before print October 1, 2009, doi: 10.1161/CIRCRESAHA.109.199513

A more recent version of this article appeared on November 6, 2009

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	Angiogenesis
	Peripheral vascular disease
	Gene therapy
	Endothelium/vascular type/nitric oxide

Submitted on April 20, 2009
Revised on September 1, 2009
Accepted on September 17, 2009

Gene Therapy With the Angiogenic Cytokine Secretoneurin Induces Therapeutic Angiogenesis by a Nitric Oxide–Dependent Mechanism

Wilfried Schgoer ; Markus Theurl ; Johannes Jeschke ; Arno G.E. Beer ; Karin Albrecht ; Roland Gander ; Song Rong ; Danijela Vasiljevic ; Margot Egger ; Anna Maria Wolf ; Silke Frauscher ; Bernhard Koller ; Ivan Tancevski ; Josef R. Patsch ; Peter Schratzberger ; Hildegunde Piza-Katzer ; Andreas Ritsch ; Ferdinand H. Bahlmann ; Reiner Fischer-Colbrie ; Dominik Wolf ; and Rudolf Kirchmair ^*

From the Department of Internal Medicine (W.S., M.T., A.G.E.B., K.A., R.G., D.V., M.E., S.F., B.K., I.T., J.R.P., P.S., A.R., R.K.), Internal Medicine 1; Tyrolean Cancer Research Institute (A.M.W., D.W.), Internal Medicine 5; and Departments of Plastic Surgery (J.J., H.P.-K.) and Pharmacology (R.F.-C.), Medical University of Innsbruck, Austria; Department of Nephrology (S.R.), Hannover Medical School, Germany; and Klinik für Innere Medizin IV (F.H.B), Universitätsklinikum des Saarlandes, Germany.

^* To whom correspondence should be addressed. E-mail: rudolf.kirchmair{at}i-med.ac.at.

Rationale: The neuropeptide secretoneurin induces angiogenesisand postnatal vasculogenesis and is upregulated by hypoxia inskeletal muscle cells.

Objective: We sought to investigate theeffects of secretoneurin on therapeutic angiogenesis.

Methodsand Results: We generated a secretoneurin gene therapy vector.In the mouse hindlimb ischemia model secretoneurin gene therapyby intramuscular plasmid injection significantly increased secretoneurincontent of injected muscles, improved functional parameters,reduced tissue necrosis, and restored blood perfusion. Increasedmuscular density of capillaries and arterioles/arteries demonstratesthe capability of secretoneurin gene therapy to induce therapeuticangiogenesis and arteriogenesis. Furthermore, recruitment ofendothelial progenitor cells was enhanced by secretoneurin genetherapy consistent with induction of postnatal vasculogenesis.Additionally, secretoneurin was able to activate nitric oxidesynthase in endothelial cells and inhibition of nitric oxideinhibited secretoneurin-induced effects on chemotaxis and capillarytube formation in vitro. In vivo, secretoneurin induced nitricoxide production and inhibition of nitric oxide attenuated secretoneurin-inducedeffects on blood perfusion, angiogenesis, arteriogenesis, andvasculogenesis. Secretoneurin also induced upregulation of basicfibroblast growth factor and platelet-derived growth factor-Bin endothelial cells.

Conclusions: In summary, our data indicatethat gene therapy with secretoneurin induces therapeutic angiogenesis,arteriogenesis, and vasculogenesis in the hindlimb ischemiamodel by a nitric oxide–dependent mechanism.

Key words: angiogenesis • endothelium • gene therapy • hypoxia • peripheral vascular disease