Hypertension, Vol 18, 774-782, Copyright © 1991 by American Heart Association
SP Tofovic, AS Pong and EK Jackson
The purpose of this study was to examine in vivo the importance of
angiotensin subtype 1 (AT1) versus subtype 2 (AT2) receptors in
spontaneously hypertensive (hypertensive) versus normotensive Wistar- Kyoto
(control) rats. Intravenous infusions of DuP 753, a selective AT1 receptor
antagonist, abolished the pressor responses to intravenous infusions of
angiotensin II in both strains, and the potency of DuP 753 in this regard
was similar in the two strains. DuP 753 also abolished angiotensin
II-induced aldosterone release in both strains; however, with respect to
inhibiting angiotensin II-induced aldosterone release, DuP 753 was more
potent in hypertensive compared with control rats. In hypertensive but not
control rats, DuP 753 inhibited angiotensin II- induced aldosterone release
at doses lower than required to inhibit angiotensin II-induced pressor
responses. Intramesenteric infusions of DuP 753 abolished mesenteric
vascular responses to intramesenteric infusions of angiotensin II with a
similar potency in both strains. In control but not hypertensive rats,
angiotensin II consistently potentiated noradrenergic neurotransmission in
the mesenteric vascular bed, and this effect of angiotensin II was
abolished by DuP 753. High doses of PD123177, a selective AT2 antagonist,
did not influence any of the aforementioned effects of angiotensin II in
either strain.(ABSTRACT TRUNCATED AT 250 WORDS)
ARTICLES
Effects of angiotensin subtype 1 and subtype 2 receptor antagonists in normotensive versus hypertensive rats
Department of Pharmacology, Vanderbilt University School of Medicine, Nashville, Tenn.
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