Hypertension, Vol 6, 660-665, Copyright © 1984 by American Heart Association
DC Eikenburg
The effects of captopril, 3 and 10 mg/kg, on vascular noradrenergic
transmission were examined in vivo in spontaneously hypertensive rats (SHR)
and normotensive Wistar-Kyoto rats (WKY). These experiments were performed
on mesenteric vascular beds perfused in situ. In WKY, 3 mg/kg captopril
failed to significantly lower mean arterial blood pressure (MAP) and also
failed to have a significant effect on the frequency- response curve to
sympathetic nerve stimulation or dose-response curve to norepinephrine (NE)
in the mesentery of WKY. In SHR mesentery, 3 mg/kg captopril failed to
alter the frequency response curve or NE dose- response curve, while it
significantly lowered MAP. The higher dose of captopril, 10 mg/kg, also
failed to lower MAP in WKY mesentery, although it caused some reduction in
pressor responses to sympathetic nerve stimulation and NE. In SHR
mesentery, 10 mg/kg captopril significantly lowered MAP and reduced pressor
responses to both nerve stimulation and NE. It should be noted, however,
that captopril lowered responses to nerve stimulation and NE to a similar
degree in both SHR and WKY, and there was no indication of a prejunctional
action on vascular noradrenergic transmission. In conclusion, although
captopril was more effective in lowering MAP in SHR than in WKY, no
evidence was found for significantly greater facilitation of vascular
sympathetic neurotransmission by endogenous angiotensin II in SHR than in
WKY, and most of the actions of captopril on vascular neurotransmission
appeared to be postjunctional in nature and unrelated to either the renin-
angiotensin system or the kallikrein-kinin system.
ARTICLES
Effects of captopril on vascular noradrenergic transmission in SHR