Literature DB >> 183514

Agonist and antimineralocorticoid activities of spirolactones.

C Sakauye, D Feldman.   

Abstract

To investigate the mechanism of action of antimineralocorticoids, a series of spirolactone analogues was evaluated for both mineralocorticoid antagonist and agonist activity. Antagonist activity was assessed by inhibition of aldosterone stimulated sodium transport employing toad bladder short-circuit current (SCC) measurements. Agonist activity was assessed in the same system by the direct effect of spirolactones on SCC. Opening of the gamma-lactone ring of a spirolactone dramatically decreased antagonist activity in the compound studied. Several C-7 chi-substitutions resulted in either enhanced or diminished activity, whereas deletion of the C-10 methyl group (i.e., 19-nor compound) had only minimal effects on antagonist potency. Agonist activity was demonstrable for three of the analogues studied: the 19-nor compound, and those containing a C-7 chi-substitution with a carboxyl isopropyl ester or a C-6-7 cyclopropyl linkage. The functional activity in toad bladder was compared to previous measurements of the relative binding affinity of the same spirolactones for mineralocorticoid receptors in rat kidney. Although there was some correlation between binding to rat kidney receptors and antagonist activity in the toad bladder, the results did not coincide in the case of the three spirolactones that possessed partial agonist activity. Some of the discrepancy may have resulted from differences between mammalian and amphibian receptors; however, intrinsic agonist activity limits antagonist potency and thus may cause a divergence between binding and functional studies limited to antagonist activity alone. Binding affinity, although indicative of total activity, fails to distinguish agonist from antagonist potency.

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Year:  1976        PMID: 183514     DOI: 10.1152/ajplegacy.1976.231.1.93

Source DB:  PubMed          Journal:  Am J Physiol        ISSN: 0002-9513


  11 in total

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Authors:  J H Ludens; D A Vaughn; D D Fanestil
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5.  Metabolic effects of high dose amiloride and spironolactone: a comparative study in normal subjects.

Authors:  J A Millar; R Fraser; P Mason; B Leckie; A M Cumming; J I Robertson
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6.  Relative potency and structure activity relationships of aldosterone antagonists in healthy man: correlation with animal experience.

Authors:  G T McInnes; J R Shelton; L E Ramsay; I R Harrison; M J Asbury; J M Clarke; R M Perkins; G R Venning
Journal:  Br J Clin Pharmacol       Date:  1982-03       Impact factor: 4.335

7.  Spironolactone. An aldosterone agonist in the stimulation of H+ secretion by turtle urinary bladder.

Authors:  A Mueller; P R Steinmetz
Journal:  J Clin Invest       Date:  1978-06       Impact factor: 14.808

8.  Spironolactone dose-response relationships in healthy subjects.

Authors:  G T McInnes; R M Perkins; J R Shelton; I R Harrison
Journal:  Br J Clin Pharmacol       Date:  1982-04       Impact factor: 4.335

9.  Effects of adrenal steroids on Na transport in the lower intestine (coprodeum) of the hen.

Authors:  W Clauss; J E Dürr; D Guth; E Skadhauge
Journal:  J Membr Biol       Date:  1987       Impact factor: 1.843

10.  Mineralocorticoid-specificity of aldosterone-induced protein synthesis in giant-toad (Bufo marinus) urinary bladders.

Authors:  M Geheb; R Alvis; E Hercker; M Cox
Journal:  Biochem J       Date:  1983-07-15       Impact factor: 3.857

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