Mechanism of Action of the Potent Sodium-Retaining Steroid 11,19-Oxidoprogesterone

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Vol. 58, Issue 1, 58-70, July 2000

Mechanism of Action of the Potent Sodium-Retaining Steroid 11,19-Oxidoprogesterone

Mario D. Galigniana, Guillermo P. Vicent, Graciela Piwien-Pilipuk, Gerardo Burton, and Carlos P. Lantos

Departamento de Química Biológica (M.D.G., G.P.V., G.P.-P, C.P.L.) and Departamento de Química Orgánica (G.B.), Facultad de Ciencias Exactas y Naturales, Universidad de Buenos Aires, and Programa de Regulación Hormonal y Metabólica-Consejo Nacional de Investigaciones Científicas y Técnicas, Ciudad Universitaria, Pabellón II, Buenos Aires, Argentina

We have demonstrated previously that a planar conformation of the molecular frame is required for steroids to acquire optimalsodium-retaining activity and binding properties to the mineralocorticoidreceptor (MR). One of the most active sodium-retaining compoundstested in those studies was 11,19-oxidoprogesterone. Despite itsbiological potency, the relative affinity of 11,19-oxidoprogesteronefor the MR is 5-fold lower than that of 21-deoxycorticosteroneand 10-fold lower than aldosterone. Such a discrepancy may beassigned to uncommon biopharmacological properties of this syntheticsteroid or an unusual molecular mechanism of action. In this work,we studied the biopharmacological and mechanistic features of11,19-oxidoprogesterone. We show that both the pharmacokineticproperties of 11,19-oxidoprogesterone and its ability to transformand translocate the MR into the nucleus are undistinguishablefrom aldosterone. However, the capability of the serine/threoninephosphatase inhibitor tautomycin to impair nuclear translocationof the aldosterone-MR complex is not observed for the 11,19-oxidoprogesterone-MRcomplex. In addition, the binding properties of both steroidsare differentially affected by modification of crucial lysyl residuesof the MR. Kinetic studies performed on the aldosterone-MR complexin the presence of low concentrations of oxidopregnane suggestthat 11,19-oxidoprogesterone may bind to the MR in a differentbinding site from the aldosterone binding pocket. Consistent withthis postulate, a biologically inactive dose of 0.6 ng of oxidopregnaneis able to potentiate the mineralocorticoid effect of a suboptimaldose ofaldosterone.

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