Lack of Anticonvulsant Tolerance to the Neuroactive Steroid Pregnanolone in Mice

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Vol. 287, Issue 2, 553-558, November 1998

Lack of Anticonvulsant Tolerance to the Neuroactive Steroid Pregnanolone in Mice

Tushar G. Kokate, Shun-Ichi Yamaguchi, Lewis K. Pannell, Umamaheswari Rajamani, David M. Carroll, Andrew B. Grossman and Michael A. Rogawski

Neuronal Excitability Section, Epilepsy Research Branch, National Institute of Neurological Disorders and Stroke (T.G.K., S.Y., D.M.C., A.B.G., M.A.R.) and Laboratory of Analytical Chemistry (L.K.P., U.R.), National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, Maryland

GABA-potentiating neuroactive steroids such as pregnanolone have potent protective effects in the pentylenetetrazol seizuretest. We sought to determine if tolerance develops to the anticonvulsantactivity of pregnanolone with chronic administration. Mice weretreated with two daily injections of a 2 × ED₅₀ dose of pregnanolone(25 mg/kg, i.p.) for 7 days. On the day after the chronic treatmentprotocol, the dose-response relationship for protection in thepentylenetetrazol seizure test was obtained. The ED₅₀ value afterthe chronic treatment protocol was not significantly differentfrom that in naive mice (12 mg/kg), indicating that tolerancedoes not develop to the anticonvulsant activity of pregnanolone.In subsequent experiments, we extended the chronic treatment protocolto 14 days with three daily injections of pregnanolone (25 mg/kg,i.p.). Again, no tolerance was observed (ED₅₀, 13 mg/kg). Theanticonvulsant activity of pregnanolone was well correlated withplasma levels in both the naive and chronically (14 day) treatedmice. The estimated plasma concentrations of pregnanolone representingthreshold (10%) protection (125-150 ng/ml) and 50% protection(575-700 ng/ml) were similar in naive and chronically treatedanimals. In both chronically treated and naive animals, plasmalevels of pregnanolone declined rapidly (t_1/2, 16-19 min)and there was a corresponding reduction in the anticonvulsantactivity. Our results with pregnanolone suggest that tolerancedoes not develop to the anticonvulsant activity of neuroactivesteroids as it does with other GABA potentiating drugs such asbenzodiazepines, supporting the potential clinical utility ofneuroactive steroids in chronic seizuretherapy.

0022-3565/98/2872-0553$03.00/0
THE JOURNAL OF PHARMACOLOGY AND EXPERIMENTAL THERAPEUTICS
Copyright © 1998 by The American Society for Pharmacology and Experimental Therapeutics

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