STEROID-HORMONES AND RECEPTORS OF THE GABA-A SUPRAMOLECULAR COMPLEX .1. BENZODIAZEPINE RECEPTOR LEVEL CHANGES IN SOME EXTRAHYPOTHALAMIC BRAIN-AREAS OF THE FEMALE RAT FOLLOWING SEX STEROID TREATMENT

The effects of sex steroid hormones on the different receptor binding sites of the GABA(A) molecule remain unclear. In this report we have d emonstrated, using autoradiography techniques, that the distribution p attern of the benzodiazepine receptors (a component of the GABA(A) mol ecule) in some extrahypothalamic brain regions is altered by both in v ivo and in vitro sex steroid hormone treatment. In vivo administration of the sex steroids estradiol and progesterone induced a significant change in [H-3]flunitrazepam (benzodiazepine agonist) binding levels i n the amygdala, and cortico and posterior brain nuclei of the female r at. In fact, elevated and diminished receptor-binding levels were obta ined in the corticomedial amygdala nucleus and in the pontine central gray matter respectively, following the administration of estradiol. S ignificant hormonal effects were also shown for animals that received only a progesterone dose, as demonstrated by the increased and decreas ed receptor levels in the basolateral amygdala nucleus and cortex lami na VI and in the substantia nigra pars reticulata, respectively. It wa s interesting, at this point, to investigate whether the hormone effec ts on [H-3]flunitrazepam binding changes might be mediated through a G ABA-dependent activity, because the benzodiazepine and GABA(A) recepto rs are coupled to a chloride ion channel in an allosteric manner. When 50 muM GABA was added to the incubation medium, substantially altered binding levels were recorded in animals that received progesterone re placement therapy only. The GABA-induced progesterone effects both inc reased substantially the binding levels in the oriens-pyramidalis CA1 layer of the hippocampus and in the intermediate gray layer of the sup erior colliculus as well as reducing receptor levels in the substantia nigra pars reticulata. Due to the significant progesterone effects on [H-3]flunitrazepam binding, we also examined whether progesterone per se or whether the potent progesterone metabolite 3alpha-hydroxy-5alph a-dihydroprogesterone was responsible for the receptor-binding changes . Addition of this progesterone metabolite not only produced greater b inding changes in brain areas that responded to the in vivo progestero ne treatment but also increased, in a GABA-dependent manner, [H-3]flun itrazepam binding levels in the lateral amygdala nucleus. These result s suggest that the anxiolytic, sedative and anti-aggressive behavioral effects, which are progesterone-dependent, are very likely mediated v ia a steroid-GABAergic interaction.