Converting enzyme blockade with MK 421 significantly lowered angiotensin II levels (P<0.001) but did not alter daily urinary sodium excretion or cumulative sodium balance compared to placebo.
RCT (n=8)
Double-blind
Randomized sequence
Does converting enzyme inhibition accelerate escape from mineralocorticoid excess in normotensive volunteers?
Suppression of circulating angiotensin II levels by ACE inhibition does not appear to be causally related to the escape from mineralocorticoid-induced sodium retention in humans.
Escape from the sodium-retaining action of mineralocorticoids coincides with the suppression of plasma renin and angiotensin II levels. The purpose of this study was to evaluate whether blockade of the renin system accelerates this escape. Eight male normotensive volunteers, aged 24--33 yr, were maintained during two subsequent periods of 12 days each, separated by 3--4 weeks, on a constant intake of sodium and potassium of 140 mmol/day. During both periods, fludrocortisone acetate (0.2 mg) was administered orally three times a day on days 4--12. In addition, on days 3--12, either a converting enzyme inhibitor (MK 421;20 mg orally, twice daily) or a placebo was added in double blind fashion and randomized sequence. During both periods, blood pressures were similar; they tended to increase slightly toward day 12. The weight increase did not differ between the two periods. With MK 421, angiotension II levels were significantly lower than with placebo on days 3--6 (P less than 0.001). On the same days, PRA was increased due to converting enzyme blockade. Despite the significantly different angiotensin II levels on days 3--6, daily urinary sodium excretion on all individual days as well as cumulative sodium balance were the same during both periods. Therefore, we could find no evidence in man that suppression of circulating angiotensin II levels is causally related to escape from mineralocorticoid excess.
Biollaz et al. (Tue,) conducted a rct in Normotensive volunteers (n=8). Converting enzyme inhibitor (MK 421) vs. Placebo was evaluated on Daily urinary sodium excretion and cumulative sodium balance. Converting enzyme blockade with MK 421 significantly lowered angiotensin II levels (P<0.001) but did not alter daily urinary sodium excretion or cumulative sodium balance compared to placebo.
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