Hypertension, Vol 3, 269-276, Copyright © 1981 by American Heart Association
SC Textor, HR Brunner and H Gavras
Interpretation of results obtained with angiotensin-converting enzyme
inhibition in hypertensive patients has been obscured by the possibility of
nonangiotensin-mediated mechanisms, particularly rats, we have compared the
effects of converting enzyme inhibition (CEI) by oral captopril
administration to those of dextrose. In this setting of constant
angiotensin II levels, any apparent effects of CEI must be mediated by a
nonangiotensin-related mechanism. Angiotensin II infusion at 30 ng/min
increased mean blood pressure by an average of 22 mm Hg. Following 7 days
of CEI, effective blockade of converting enzyme was established both by a
10-fold elevation of vasodepressor sensitivity to exogenous bradykinin and
a markedly decreased plasma converting enzyme activity. On the ninth day of
angiotensin II infusion, mean arterial pressure, heart rate, and plasma
renin activity were not different between CEI and dextrose-treated groups.
Similarly, blockade of angiotensin II by saralasin induced a comparable
fall in blood pressure in both groups. Metabolic studies also revealed no
long-term differences in water and food intake, weight change, or sodium
and potassium metabolisms. These findings suggest that, in the continued
presence of angiotensin II, there is no detectable hemodynamic or metabolic
effect of chronic converting enzyme inhibition, and therefore that
bradykinin plays little or no role in its long-term antihypertensive
action.
ARTICLES
Converting enzyme inhibition during chronic angiotensin II infusion in rats. Evidence against a nonangiotensin mechanism
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