Barbiturate Anesthesia Blocks the Positive Feedback Effect of Progesterone, but not of Estrogen, on Luteinizing Hormone Release in Ovariectomized Guinea Pigs*

Abstract

In female rats, pentobarbital anesthesia blocks estrogen- or progesterone-induced LH release. This experiment was designed to test the effects of barbiturates on the steroidinduced LH surge in the female guinea pig. Animals were housed in a light-controlled room (lights on from 0600–1800 h) and ovariectomized 2 weeks before the experiment. Blood samples were obtained through a chronic indwelling catheter. Plasma LH was estimated by RIA. Estradiol benzoate alone (EB; 10 fig injected sc at 1000 h) or EB (1.5 μg injected sc at 1000 h) folowed by progesterone (P4; 1.0 mg sc) 30 h later consistently induced an LH suige between 33–42 h after EB (10 μg) or between 6–12 h after P4. Multiple injections of pentobarbital (30 mg/kg), starting at 30 h after EB, or a single injection of phenobarbital (100 mg/kg), starting at 27 h after EB, were given before the expected LH surge in both EB alone and EB plus P₄-treated animals. Animals slept for about 15 h under multiple injections of pentobarbital and for about 35 h under a single injection of phenobarbital. In all animals (n = 11), pentobarbital was effective in blocking the P₄-induced LH surge completely. On the other hand, both pentobarbital and phenobarbital anesthesia failed to block the estrogen-induced LH surge; 7 of 14 and 6 of 9 animals, respectively, had LH surges during the expected period and 4 of 14 and 3 of 9 animals, respectively, had LH surges 24 h after the expected period. Thus, it is suggested that the mechanism of action by which P4 facilitates LH release differs from that of estrogen. P₄ may act primarily on higher brain structures and for a limited period of time. However, estrogen (10 μg) may act primarily on the medial basal hypothalamus as well as on the pituitary and for a longer period so that LH release can occur during the time of anesthesia or 24 h after the expected period.