Abstract
Heroin intake decreases during the proestrus phase of the estrous cycle in female rats. Circulating concentrations of both estradiol andprogesterone peak during proestrus, and it is not known which of these hormones, or their combination, are responsible for these effects. The purpose of this study was to determine the effects of estradiol, progesterone, and their combination on heroin self-administration in femalerats. In Experiment 1, the estrous cycle of intact female rats was tracked daily. If a rat was in proestrus, either the estrogen receptor antagonist,raloxifene, the progesterone receptor antagonist, mifepristone, or their combination was administered 30 min prior to a heroin self-administration session. InExperiment 2, separate groups of ovariectomized female rats were treated chronically with exogenous estradiol, progesterone, estradiol + progesterone, orvehicle, and heroin intake was examined over a 100-fold dose range. In Experiment 1, raloxifene, but not mifepristone, significantly blocked proestrus-associated decreases in heroin intake. In Experiment 2, estrogentreatedrats self-administered less heroin than any other group and significantly less heroin than rats treated with progesterone. These data suggest that (1) estradiol but not progesterone is responsible for proestrus-associated decreases in heroin intake and (2) estradioldecreases heroin intake relative to progesterone. These data differ from those reported previously with stimulants and suggest that estrogen-basedpharmacotherapies may be of value to women with opioid use disorder.
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