ACTIVATION OF GABAA RECEPTORS AND INHIBITION OF NEUROSTEROID SYNTHESIS HAVE SEPARABLE ESTROUS-DEPENDENT EFFECTS ON BINGE DRINKING IN FEMALE MICE

Abstract

Alcohol concentrations relevant to the beginning stages of binge intoxica-tion may selectively activate GABAA receptor subtypes expressing δ-subunit proteins (δ-GABAAR). Indeed, administration of agonists that interact with these δ-GABAAR prior to alcohol access, can abolish binge drinking behavior (Melon and Boehm, 2011). Unfortunately, our ability to manipulate binge drinking in females is dependent upon estrous phase. The present experi-ments were designed to clarify the estrous-dependent effects of activation of δ-GABAAR on binge drinking. Specifically, we were interested in demonstrat-ing whether females display more persistent binge drinking as a function of cycle-dependent changes in the synthesis of endogenous neurosteroids that modulate δ-GABAAR. Using the Drinking-in-the-Dark binge-drinking model, regularly cycling female mice were given 2 hours of daily access to alcohol (20%v/v). Vaginal cytology was assessed after each drinking session to track estrous status. In experiment 1, animals were administered gaboxadol (an agonist with high affinity for δ-GABAAR) prior to their 8th day of access. In experiment 2, these methods were repeated, but mice received vehicle or finasteride (a neurosteroid synthesis inhibitor) 22hr prior to their 8th day of access. Results from experiment 1 demonstrated that diestrus females were insensitive to the significant gaboxadol-induced decrease in binge drinking observed for proestrus, estrus and metestrus females. In experiment 2, ve-hicle and finasteride treated diestrus females exhibited gaboxadol-induced reduction of their binge drinking. Surprisingly, finasteride pretreatment sig-nificantly reduced binge drinking for estrus females. These studies suggest that ovarian-linked changes to extrasynaptic GABAA R and to neurosteroid activity may be important factors in the binge consumption of alcohol for females. Future studies will further explore the role that acute stress during diestrus may play in inhibiting the effects of δ-GABAA R activation on binge drinking.