Functional role of endothelin ET A and ET B receptors in venous and arterial smooth muscle

Abstract

The functional importance of endothelin ET A and ET B receptors in selected arterial and venous smooth muscle preparations was characterized. Endothelin-1 induced force in the saphenous and jugular veins is normally mediated by endothelin ET B-like receptors. However, desensitization or pharmacological block of these receptors reveals an endothelin ET A receptor population that is of sufficient size to mediate full endothelin-1-evoked force. Block of either endothelin ET A or endothelin ET B receptors alone is insufficient to antagonize endothelin-1-evoked force in saphenous vein. Endothelin-1-induced force in hamster aorta may also be mediated by activation of both endothelin ET A and ET B receptors. However, activation of endothelin ET B-like receptors alone is insufficient to generate a full endothelin-1 response. Sarafotoxin S6c treatment, to desensitize endothelin ET B receptors, failed to affect the responses of rat aorta and rabbit carotid artery to endothelin-1 or endothelin ET A receptor antagonists. These findings indicate that selective endothelin receptor antagonists will vary enormously in their efficacy against endothelin-induced force in different vascular beds.