Effects of estrogen deprivation on brain estrogen and progestin receptor levels and the activation of female sexual behavior

Ovariectomy (OVX) in rats is followed by a decline in behavioral sensitivity to combined estrogen and progesterone therapy. The purpose of this study was to further characterize this behavioral change, and to explore its biochemical basis in terms of estrogen and progesterone receptor concentrations in the brain. Sexually inexperienced female rats were used 5 (short-term) or 35 (long-term) days after OVX. Short- and long-term OVX animals were injected with estradiol-17β (E₂; 36 μg/kg body wt, iv) then subjected to one of the following three treatment schedules. (1) Animals were treated with progesterone (1 mg, sc in oil) 20–21 hr after E₂ injection, then tested at 24 hr for female sexual behavior. (2) One or twelve hours after the E₂, cell nuclear estrogen receptors (ER_n) were measured in the pituitary (PIT) and pooled preoptic area and mediobasal hypothalamus (POA-MBH). (3) Twenty-four hours after E₂, progestin receptor (PR_c) concentrations were measured in cytoplasmic fractions prepared from PIT and POA-MBH. Long-term OVX animals showed a reduced capacity to exhibit proceptive and receptive sexual behavior, and a lower PR_c level in the PIT and POA-MBH 24 hr after E₂ injection than animals that had been OVX for only 5 days. However, no differences were observed between long- and short-term OVX rats with respect to ER_n concentrations in PIT and POA-MBH cell nuclei 1 or 12 hr after E₂. Thus, it appears that the decline in behavioral responsiveness to E₂ which occurs after ovariectomy cannot be attributed to a decrease in the ability of E₂ to translocate estrogen receptors into POA-MBH cell nuclei, but is more probably associated with a change in the biochemical processes subsequent to ER_n binding. One of these processes may well be the induction of cytoplasmic progestin receptors.