Relative importance of the adenohypophyseal and gonadal sites in inhibitory action of LHRH agonists.

Abstract

Assessment of the role of endogenous LH release and direct gonadal action of LHRH agonists in the loss of gonadal LH receptors induced by treatment with gonadotropin-releasing peptides was first made by comparing the effect of single administration of 1 �g of ID-Ala’, des-Gly-NH2 ‘#{176} I LHRH ethylamide, ED-Ala’) LHRH-EA, 12 h before or immediately after hypophysectomy (HYPOX) on LH receptor levels measured 48 h after surgery in male and female adult rats. While administration of the LHRH agonist before HYPOX leads to a 50% loss of testicular LH receptors, only a 20% decrease is seen in HYPOX animals, thus suggesting a predominant role of endogenous LH release in the desensitization process in male animals. Treatment with increasing doses (1 to 100 ng/day) of another LHRH agonist, [D-Ser(TBU)’ I LHRH-EA, causes a 90% loss of testicular LH receptors in intact rats at the highest dose used (100 ng daily for 9 days) while the same treatment decreases LH receptors by only 35% in HYPOX animals. As measured by the steroidogenic response to 10 �g 0LH in vivo, while treatment of intact animals with [D-Ser(TBU)’ I LHRHEA leads to a marked blockage of the testicular steroidogenic pathway at the level of 17-hydroxylase and 17,20-desmolase activities with a corresponding increase of 5o-reductase activity, minimal or no signs of changes of enzymatic activity are seen after identical treatment in HYPOX animals. Chronic treatment (1 month) with the LHRH agonist in intact rats leads to degenerative changes of the seminiferous tubules, while no effect is observed in HYPOX animals, thus suggesting the essential role of the pituitary gland. Moreover, adrenalectomy does not influence the inhibitory effect of treatment with LHRH agonists on the loss of testicular LH receptors in HYPOX animals, thus eliminating the role of the adrenals in the action of LHRH agonists. Contrary to the results obtained in male animals, single administration of the LHRH agonist in female rats has similar inhibitory effects on ovarian gonadotropin receptors when administered either before or after hypophysectomy. Moreover, treatment with increasing doses of ED-Ser(TBU)’ I LHRH-EA leads to a similar inhibition of ovarian LH receptor levels in intact and HYPOX female animals. The present data show that LHRI-I agonist-induced endogenous LH release plays a predominant role in the desensitizing effect of treatment with LHRH agonists on testicular LH receptors and steroidogenesis as well as on inhibition of spermatogenesis; in the female, the direct gonadal effect, at least on LH and FSH receptors, appears to play a more important role than in male animals.