Blockade of the Spontaneous Midcycle Gonadotropin Surge in Monkeys by RU 486: A Progesterone Antagonist or AgonistÓ*

Abstract

Preovulatory ovarian secretion of progesterone (P₄), several hours before the onset of the typical midcycle gonadotropin surge, occurs in humans and monkeys. We investigated the potentially obligatory role of preovulatory P₄ secretion in stimulating the midcycle LH surge by administering a potent P₄ antagonist, RU 486(17β-hgydroxy-lllβ-[4-dimethylaminophenyl-l]17α[prop-l-ynyl]estra-4,9-dien-3-one), to sexually mature, normally ovulatory cynomolgus monkeys on days 10–12 of the menstrual cycle (n = 18). Monkeys were randomized to receive 1) RU 486 alone (5 mg/day, im; group I); 2) RU 486 plus dexamethasone (1 mg/day, im; group II); 3) dexamethasone alone (group III); or 4) vehicle (ethanol; 0.5 ml; group IV). Before drug treatment, the follicular phases were quite similar among groups. The administration of RU 486 blocked (delayed) the expected gonadotropin surge, despite rising estrogen concentrations (>250 pg/ml). The expected LH surge was delayed by RU 486 (n = 5) or RU 486 with dexamethasone (n = 3) until 36 ± 7 (±SEM) and 27 ± 8 days in groups I and II, respectively. In contrast, groups III (n = 3) and IV (n = 5) had timely midcycle surges after the administration of dexamethasone or vehicle alone (4 ± 2 and 6 ± 2 days, respectively). The intermenstrual interval was lengthened by RU 486 administration in both group I and II animals (61 ± 6 and 54 ± 6 days) compared to controls (30 ± 2; P < 0.0001). In summary, RU 486 effectively blocked imminent midcycle gonadotropin surges, delayed subsequent folliculogenesis, and significantly extended the menstrual cycle length. If RU 486 acted as a pure P₄ antagonist, then P₄ is necessary for timely midcycle gonadotropin surges to occur. However, recent evidence showing agonistic properties of RU 486 (in the virtual absence of P₄) at both endometrial and pituitary levels may favor a P₄-like (agonistic) blockade of the estrogen-induced FSH/LH surges by RU 486. (J Clin Endocrinol Metab63: 1270, 1986)