AJP - Heart and Circulatory Physiology, Vol 250, Issue 5 755-H760, Copyright © 1986 by American Physiological Society
Vasoactive intestinal peptide: vasodilatation and cyclic AMP generation
P. Ganz, A. W. Sandrock, S. C. Landis, J. Leopold, M. A. Gimbrone Jr and R. W. Alexander
Vasoactive intestinal peptide (VIP) is a putative neurotransmitter that
causes vasodilation when injected intravenously. To learn more about the
vasodilator actions of VIP, studies were performed on the rat mesenteric
arterial bed and on cultured smooth muscle cells derived from both the rat
mesenteric artery and aorta. In isolated perfused rat mesenteric artery
beds, VIP caused relaxation at the threshold concentration of less than 1
nM and a maximal fall in perfusion pressure similar to that obtained with
isoproterenol. VIP stimulated adenylate cyclase in cultured vascular smooth
muscle cells in a concentration range of 10(-10)-10(-6) M; maximum activity
was increased 2.7 +/- 0.6- and 3.4 +/- 0.4-fold above basal in mesenteric
and aortic smooth muscle cells, respectively. The threshold and the
half-maximal concentrations of VIP for adenylate cyclase stimulation were
more than 50-fold lower than those for both prostaglandin E1 and
isoproterenol in cultured mesenteric and aortic cells. Similar effects on
cyclic AMP generation in response to VIP were observed in isolated rat
mesenteric artery rings. Immunocytochemical examination of the rat
mesenteric artery bed in situ demonstrated dense innervation of small- and
medium-size vessels with nerve fibers containing VIP-like immunoreactivity.
Thus VIP is present in the rat mesenteric artery, a peripheral arterial
bed, and is a potent vasodilator that can activate vascular smooth muscle
adenylate cyclase and thus potentially contribute to the regulation of
vascular tone.
