Marshall J C, Case G D, Valk T W, Corley K P, Sauder S E, Kelch R P
J Clin Invest. 1983 Feb;71(2):248-57. doi: 10.1172/jci110765.
Prepubertal girls and gonadotropin-releasing hormone (GnRH)-deficient females secrete follicle-stimulating hormone (FSH) preferentially in response to intravenous GnRH. With continued pulsatile GnRH stimulation, FSH secretion is reduced when plasma estradiol (E2) is increasing. To delineate the mechanisms involved in these changing gonadotropin responses, e studied the effect of low dose (0.025 micrograms/kg) pulsatile injections of GnRH in females with varying degrees and/or duration of endogenous GnRH deficiency (idiopathic panhypopituitarism, PHP; isolated growth hormone deficiency, IGHD; isolated gonadotropin deficiency, IGD; and anorexia nervosa, AN; both at low body weight and after weight regain). In patients presumed to have the most severe GnRH deficiency (PHP), responses of both FSH and luteinizing hormone (LH) were small and delayed, and no increase in plasma estradiol occurred during the 5 d of GnRH injections. In patients previously exposed to prepubertal or adult levels of endogenous GnRH secretion (IGHD, IGD, AN at low body weight), a rapid initial FSH response occurred that subsequently declined when plasma estradiol rose to concentrations greater than 40-50 pg/ml. Prior therapy with estrogen (micronized estradiol, Estrace) abolished FSH responses but LH responses were only slightly impaired. The degree of FSH response was dependent upon the time of initiation of estrogen relative to the onset of GnRH injections. Administration of estrogen after the first GnRH injection inhibited gonadotropin responses, whereas later estrogen therapy (after 1 d of GnRH pulses) blunted the GnRH induced FSH secretion without significantly impairing the LH response. In weight-regained anorexic patients who had spontaneous pulsatile LH secretion and a mean basal plasma estradiol concentration of 53 +/- 15 pg/ml, administration of GnRH pulses did not change plasma LH and a minimal FSH response was seen. The data indicate that the pattern of gonadotropin responses to low dose GnRH injections depends upon the degree of previous exposure of the pituitary to endogenous GnRH. Furthermore, estradiol selectively inhibits FSH secretion by a direct action on the pituitary gland. This action of estradiol provides an explanation for the selective reduction in FSH responses to GnRH seen during pubertal maturation in girls and during the mid-follicular stage of the menstrual cycle.
青春期前女孩和促性腺激素释放激素(GnRH)缺乏的女性在静脉注射GnRH后优先分泌促卵泡生成素(FSH)。随着持续的GnRH脉冲刺激,当血浆雌二醇(E2)升高时,FSH分泌减少。为了阐明这些促性腺激素反应变化所涉及的机制,我们研究了低剂量(0.025微克/千克)GnRH脉冲注射对不同程度和/或持续时间的内源性GnRH缺乏女性(特发性全垂体功能减退症,PHP;孤立性生长激素缺乏症,IGHD;孤立性促性腺激素缺乏症,IGD;神经性厌食症,AN;均处于低体重状态和体重恢复后)的影响。在推测为GnRH缺乏最严重的患者(PHP)中,FSH和促黄体生成素(LH)的反应均较小且延迟,并且在GnRH注射的5天内血浆雌二醇没有升高。在先前暴露于青春期前或成人水平内源性GnRH分泌的患者(IGHD、IGD、低体重的AN)中,最初出现快速的FSH反应,随后当血浆雌二醇升至大于40 - 50 pg/ml的浓度时反应下降。先前用雌激素(微粒化雌二醇,Estrace)治疗消除了FSH反应,但LH反应仅略有受损。FSH反应的程度取决于相对于GnRH注射开始时间的雌激素起始时间。在第一次GnRH注射后给予雌激素抑制促性腺激素反应,而后期雌激素治疗(在GnRH脉冲1天后)减弱GnRH诱导的FSH分泌,而不显著损害LH反应。在体重恢复的神经性厌食症患者中,这些患者有自发性LH脉冲分泌且平均基础血浆雌二醇浓度为53±15 pg/ml,给予GnRH脉冲未改变血浆LH,仅出现最小的FSH反应。数据表明,促性腺激素对低剂量GnRH注射的反应模式取决于垂体先前暴露于内源性GnRH的程度。此外,雌二醇通过对垂体的直接作用选择性抑制FSH分泌。雌二醇的这种作用解释了在女孩青春期成熟期间以及月经周期卵泡中期阶段观察到的FSH对GnRH反应的选择性降低。
