Relationship of Plasma Aldadiene Levels and Antimineralocorticoid Effects of Spironolactone in the Laboratory

Kagawa, C. M.; Bouska, D. J.; Anderson, Margaret

doi:10.3181/00379727-115-29052

Cited by 27 publications

(15 citation statements)

References 2 publications

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“…The mean and SEM results in the 12 subjects for sodium excretion, potassium excretion, Na/K ratio, log 10 10 Na/K, and urine volume are shown in Table I. This table also shows the significance levels for tests of linearity of the log dose-response trends, for the slope of the log dose-response trends, and for tests of parallelism of the log dose-responses of the two drugs.…”

Section: Resultsmentioning

confidence: 99%

“…In the early stages of evaluation of prorenoate, we wished, for safety reasons, to observe the effects of single doses of the drug before proceeding to repeated dosing. Kagawa and his coworkers 10,11 have shown that dose-response curves can be obtained using single doses of spirolactones in laboratory animals, and that this method of bioassay yields valid estimates of relative potency for these drugs. We 17 and others 20 have shown that the procedure of Ross 18 can be adapted to allow testing of single doses of aldosterone antagonists in normal man.…”

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confidence: 99%

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Relative potency of prorenoate and spironolactone in normal man

Ramsay¹,

Harrison²,

Shelton³

et al. 1975

Clin Pharma and Therapeutics

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The potency of single doses of a new aldosterone antagonist, prorenoate, in reversing the renal effects of the synthetic mineralocorticoid fludrocortisone was compared to that of spironolactone in a double-blind balanced crossover study in 12 healthy subjects. The potency of prorenoate potassium as related to elevation of the urinary log 10 10 Na/K ratio (2.69:1) and as related to potassium retention (3.75:1) was significantly higher than that of spironolactone. Prorenoate produced greater natriuresis (1.64:1) but the difference was not significant. There was evidence for a qualitative difference between spironolactone and prorenoate; the latter significantly more potent in retaining potassium than in increasing sodium excretion. The simple methodology described is based on standard bioassay principles, yielded a valid and sensitive comparison of the two drugs, and should prove useful in the evaluation of other aldosterone antagonists.

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Section: Resultsmentioning

confidence: 99%

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confidence: 99%

Relative potency of prorenoate and spironolactone in normal man

Ramsay¹,

Harrison²,

Shelton³

et al. 1975

Clin Pharma and Therapeutics

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“…The two drugs must have a relative potency or, if this assumption is incorrect, the hypothesis that canrenone is responsible for the activity of both drugs must be rejected. (Kagawa et al, 1964). These workers treated rats and dogs with spironolactone and canrenone at doses which yielded similar levels of canrenone in plasma, and simultaneously measured the potency of the compounds in reversing the renal effects of deoxycorticosterone acetate.…”

Section: Discussionmentioning

confidence: 99%

“…The 7a-acetylthio substituent is removed completely from 80% of the administered dose (Sadee, Dagcioglu & Schr6der, 1973) yielding canrenone (other names: aldadiene, SC-9376) (Figure 1) as the principal non-conjugated metabolite in plasma. Canrenone is active as a mineralocorticoid antagonist in animals (Kagawa, Bouska & Anderson, 1964) and has been proposed as the principal pharmacologically active agent after administration of spironolactone to man (Sadee, Dagcioglu & Schr6der, 1972).…”

Section: Introductionmentioning

confidence: 99%

Canrenone—the Principal Active Metabolite of Spironolactone?

Ramsay¹,

Shelton²,

Wilkinson³

et al. 1976

Brit J Clinical Pharma

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I The properties of the aldosterone antagonists spironolactone and potassium canrenoate in tablet formulations were examined in two studies in healthy subjects, the first study comparing levels of their common major metabolite, canrenone, in plasma and the second study comparing the pharmacological activity of the two drugs in reversing the renal effects of the synthetic mineralocorticoid fludrocortisone. 2 At equal dosage by weight potassium canrenoate yielded peak levels and areas under the curve for canrenone in plasma which were significantly lower than those for spironolactone, and the peak level of canrenone was reached significantly later. Comparison with published work suggests that the experimental formulation of potassium canrenoate had low bioavailability. 3 Spironolactone produced statistically valid log dose-response curves against fludrocortisone as regards sodium excretion, potassium retention and increased urine sodium to potassium ratio. There was no significant log dose-reponse after potassium canrenoate, and a statistically valid estimate of relative potency could not be obtained. 4 The results of the two studies seem inconsistent with the view that canrenone alone is responsible for the pharmacological activity of both drugs, and suggest that a significant part of the activity of spironolactone may be attributable to metabolites other than canrenone.

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“…From a study of subjects receiving spironolactone who had reached a steady state, Ramsay et al (1977) concluded that canrenone was the principal active metabolite of spironolactone. Conversely, in assessing the antimineralocorticoid activity of a single dose of spironolactone it has been shown that spironolactone was significantly more potent than predicted from the plasma canrenone levels both in human subjects (Ramsay et al, 1976) and animals (Kagawa, Bouska & Anderson, 1964). Furthermore, with a more selective chromatographic assay for canrenone (Dahlof et al, 1979;Ashbagen et al, 1979) the contribution of canrenone to the antimineralocorticoid effect of spironolactone is substantially lower than previously assumed from the fluorimetric method of Gochman & Gantt (1962).…”

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confidence: 99%