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Effect of angioplasty and grafting on porcine vascular nerves: a potential neurotropic role for endothelin-1

Published online by Cambridge University Press:  01 April 1998

M. R. DASHWOOD
Affiliation:
Department of Physiology, Royal Free Hospital School of Medicine, Rowland Hill Street, London NW3 2PF, UK
G. D. ANGELINI
Affiliation:
Bristol Heart Institute, Bristol Royal Infirmary, Bristol BS2 8HW, UK
D. MEHTA
Affiliation:
Bristol Heart Institute, Bristol Royal Infirmary, Bristol BS2 8HW, UK
J. Y. JEREMY
Affiliation:
Bristol Heart Institute, Bristol Royal Infirmary, Bristol BS2 8HW, UK
K. MUENTER
Affiliation:
Preclinical Cardiology, Knoll AG, Postfach 2108 05, 67008 Luwigshafen, Germany
M. KIRCHENGAST
Affiliation:
Preclinical Cardiology, Knoll AG, Postfach 2108 05, 67008 Luwigshafen, Germany
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Abstract

The most commonly performed procedure for treating coronary artery stenosis is percutaneous transluminal coronary angioplasty (PTCA) and, where the vessel lumen is severely narrowed, coronary artery bypass grafting (CABG). In PTCA, regions of atherosclerotic plaques are disrupted, and the vessel lumen increased by inflating a balloon catheter. In CABG an autologous saphenous vein into coronary artery interposition graft is performed in order to bypass occluded regions of epicardial coronary arteries. Both interventions cause varying degrees of vascular damage and the long-term efficacy of these procedures is limited by a high incidence of neointimal formation and subsequent vascular restenosis (Bach et al. 1994; Bryan & Angelini, 1994).

The endothelium-derived constrictor peptide, endothelin-1 (ET-1) (Yanagisawa et al. 1988), also possesses mitogenic activity on vascular smooth muscle cells (Hirata et al. 1989) and has been suggested as playing a role in atherosclerosis (Dashwood et al. 1993; Zeiher et al. 1994) and intimal hyperplasia (Dashwood et al. 1993; Douglas et al. 1994).

Type
Correspondence
Copyright
© Anatomical Society of Great Britain and Ireland 1998

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