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Am J Physiol Regul Integr Comp Physiol 274: R903-R911, 1998;
0363-6119/98 $5.00
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Vol. 274, Issue 4, R903-R911, April 1998

Neurosteroid modulation of arterial baroreflexsensitive neurons in rat rostral ventrolateral medulla

J. D. Laiprasert, R. C. Rogers, and C. M. Heesch

Department of Physiology, The Ohio State University, Columbus, Ohio 43210-1218

The major metabolite of progesterone, 3alpha -OH-dihydroprogesterone (3alpha -OH-DHP), is the most potent endogenous positive modulator of central nervous system GABAA receptors. Acute intravenous administration of 3alpha -OH-DHP to virgin female rats potentiates arterial baroreflex sympathoinhibitory responses. The current experiments tested the possibility that circulating 3alpha -OH-DHP potentiates central GABAergic influences in the rostral ventrolateral medulla (RVLM). The unit activity of spontaneously active, spinally projecting, and arterial pressure-sensitive neurons was recorded in the RVLM of urethan-anesthetized rats. Arterial pressure sensitivity of RVLM neurons was tested before (control) and 10 min after bolus injection (44 µl iv) of 3alpha -OH-DHP (1.12 µg/kg, n = 19) or vehicle (40% beta -cyclodextrin, n = 8). Both threshold pressure and saturation pressure for inhibition of RVLM neurons were decreased after acute administration of a physiological dose of 3alpha -OH-DHP (1.12 µg/kg iv), which produces plasma concentrations similar to those seen during pregnancy (20-30 ng/ml), suggesting potentiated responsiveness to endogenously released GABA. Following suppression by 3alpha -OH-DHP, high doses of the inactive stereoisomer 3beta -OH-DHP (112-224 µg/kg iv; n = 8) restored unit activity, presumably by displacing 3alpha -OH-DHP from the neurosteroid binding site on GABAA receptors.

gamma -aminobutyric acid; baroreflex; progesterone


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