9 research outputs found
Estimation of a natural spirolactone derivative in normal and hypertensive man by gas-liquid chromatograpby
No full textIdentification of unknown steroids by NMR spectroscopy and mass spectrometry: discovery of a natural spirolactone derivative in man and animal
No full textEstimation of 18-hydroxy-11-deoxycorticosterone (18-OH-DOC) in human plasma and urine including a comparison of various techniques
No full text3. The binding of 18-hydroxydeoxycorticosterone (18-OH-DOC) of 18-hydroxyprogesterone (18-OH-progesterone) of a new urinary 18-hydroxysteroid and a set of fluorinated steroids to mineralocoiticoid and ghicocorticoid receptors in the rat kidney
No full textEffect of Various 6-Dehydro-Corticosteroids, 9, 11-Dehydro-Doca and 9 Alpha-Fluoro-Doca on the Fluxes of Sodium and Potassium
Full text linkpeer reviewedThe introduction of a double bond at carbons 6 and 7 (6-dehydro-derivatives) of deoxycorticosterone acetate (DOCA), cortisol-21-acetate, 9 alpha-fluorocortisol-21-acetate (9 alpha-F-C-ac) and aldosterone-21-acetate substantially reduces affinity for Type II receptors but not for Type I receptors. Such a modification changes the effect of these steroids on urinary excretion of Na+ and K+. 6-Dehydro-derivatives will thus bind preferentially to receptor Type I inducing the retention of sodium and compete with mineralocorticoids for such receptors. The increase in both natriuresis and kaliuresis when corticosteroids and their 6-dehydro-derivatives are administered together may be interpreted as evidence for a Type II receptor mediation of those ion fluxes. The ionic changes are not mediated by the (Na+ + K+)-ATPase system. The fluoration at 9 and the dehydrogenation at C9C11 of DOCA result in a strong increase of binding to Type I receptor and of sodium retention
Arguments for the Existence of an Endogenous Inhibitor of Renal Na-K Atpase with Steroid Structure and Natriuretic Action
Full text linkIn order to explain the opposite effect of 6,7-dihydroxylated isomers of 6, 7 - dihydrocanrenone on the urinary sodium and potassium excretion, we have tested the effect of these substances isolated from human urine on the Na(+)-K+ pump from different tissue preparation: rabbit kidney slices as well as NA-K ATPase purified from the kidney. Our results show an inhibition of pump as well as enzyme activity by the 6 beta 7 alpha isomer while the 2 other isomers are either uneffective or slightly stimulating. The 6 beta 7 alpha dihydroxy-6, 7-dihydrocanrenone could be one of the plasma ouabain-like substance incriminated in the pathogenesis of volume-expanded hypertension
Arguments for the existance of an endogenous inhibitor of the renal Na-K ATPase enzyme with steroid structure and natriuretic action
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