PST 2238: A New Antihypertensive Compound that Modulates Na,K-ATPase in Genetic Hypertension

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Vol. 288, Issue 3, 1074-1083, March 1999

PST 2238: A New Antihypertensive Compound that Modulates Na,K-ATPase in Genetic Hypertension

P. Ferrari, M. Ferrandi, G. Tripodi, L. Torielli, G. Padoani, E. Minotti, P. Melloni and G. Bianchi

Prassis Research Institute Sigma-Tau (P.F., L.T., M.F., G.T., G.P., E.M., P.M.), Milan, Italy; and Chair of Nephrology, Division of Nephrology and Hypertension, University of Milan and S. Raffaele Hospital (G.B.), Milan, Italy

A genetic alteration in the adducin genes is associated with hypertension and up-regulation of the expression of renal Na,K-ATPasein Milan-hypertensive (MHS) rats, in which increased ouabain-likefactor (OLF) levels are also observed. PST 2238, a new antihypertensivecompound that antagonizes the pressor effect of ouabain in vivoand normalizes ouabain-dependent up-regulation of the renal Na-Kpump, was evaluated for its ability to lower blood pressure andregulate renal Na,K-ATPase activity in MHS genetic hypertension.In this study, we show that PST 2238, given orally at very lowdoses (1 and 10 µg/kg for 5-6 weeks), reduced the developmentof hypertension in MHS rats and normalized the increased renalNa,K-ATPase activity and mRNA levels, whereas it did not affecteither blood pressure or Na,K-ATPase in Milan-normotensive (MNS)rats. In addition, a similar antihypertensive effect was observedin adult MHS rats after a short-term treatment. In cultured ratrenal cells with increased Na-K pump activity at V_max due to overexpressionof the hypertensive variant of adducin, 5 days of incubation withPST 2238 (10^10--10⁹ M) lowered the pump rate to the level of normal wild-type cells,which in turn were not affected by the drug. In conclusion, PST2238 is a very potent compound that in MHS rats reduces bloodpressure and normalizes Na-K pump alterations caused by a geneticalteration of the cytoskeletal adducin. Because adducin gene mutationshave been associated with human essential hypertension, it issuggested that PST 2238 may display greater antihypertensive activityin those patients carrying such a geneticalteration.

0022-3565/99/2883-1074$03.00/0
THE JOURNAL OF PHARMACOLOGY AND EXPERIMENTAL THERAPEUTICS
Copyright © 1999 by The American Society for Pharmacology and Experimental Therapeutics

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