AJP - Heart and Circulatory Physiology, Vol 232, Issue 3 305-H310, Copyright © 1977 by American Physiological Society
Blood vessel-hormone interactions: angiotensin, bradykinin, and prostaglandins
A. L. Blumberg, S. E. Denny, G. R. Marshall and P. Needleman
Isolated Krebs-perfused rabbit-mesentery blood vessels release a
prostaglandin E-like substance (PGE) when treated with angiotensin II,
angiotensin I, arachidonic acid, or bradykinin. The specific competitive
antagonist [Sar1,Ile8]angiotensin II, was found to inhibit angiotensin
II-induced PGE release. The angiotensin antagonist did not block PGE
release by bradykinin, whereas indomethacin blocked PGE release induced by
all agonists. SQ-20881, the converting-enzyme and bradykininase inhibitor,
decreased the PGE release by angiotensin I, enhanced the release by
bradykinin, and did not affect release by angiotensin II. Pressor and
depressor responses were obtained in mesenteric preparations constricted by
epinephrine to a pressure of 60 mmHg. Angiotensin II induced an initial
increase in mesenteric vascular resistance followed by a depressor response
below basal pressure. The pressor responses were enhanced by indomethacin
and the depressor responses were eliminated. Bolus injections of both
bradykinin and arachidonic acid produced decreases in perfusion pressure,
but indomethacin completely inhibited only the arachidonic acid-induced
responses while only diminishing bradykinin-induced responses. The ability
of angiotensin to increase mesenteric vascular resistance and to release
PGE which decrease vascular resistance is discussed.
