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人类卵泡期孕酮脉冲式分泌的来源。

The source of pulsatile secretion of progesterone during the human follicular phase.

作者信息

Judd S, Terry A, Petrucco M, White G

机构信息

Department of Medicine, Flinders Medical Centre, Bedford Park, South Australia.

出版信息

J Clin Endocrinol Metab. 1992 Feb;74(2):299-305. doi: 10.1210/jcem.74.2.1730808.

Abstract

This study was designed to establish the normal pattern of serum progesterone and the origin of its secretion during the follicular phase of the normal menstrual cycle. In the first study, 12 normal women were studied on 3 occasions each at different times during a single follicular phase. Serum samples were collected every 10 min over 8 h, for 6 h before and 2 h after an injection of naloxone (5 mg iv). The mean serum progesterone remained constant (0.9 nmol/L) across the follicular phase until just before ovulation; individual subjects showed pulsatility of progesterone (1-6 pulses/6 h) but there was no relationship of this to LH pulsatility and no variation of progesterone pulsatility across the follicular phase. Naloxone caused an increase in the mean serum progesterone in the early follicular phase to 1.9 +/- 0.7 nmol/L and in the mid and late follicular phase to 2.1 +/- 0.7 nmol/L and 3.4 +/- 2.5 nmol/L, respectively. The second study was performed to assess the contribution of the residual corpus luteum and the developing follicle to the pulsatile secretion of progesterone. Seven anovulatory women with low levels of serum LH and absent LH pulsatility were studied before and after clomiphene (100 mg/day for 5 days) by collecting blood samples every 15 min for 6 h before GnRH (10 mg iv) and for 2 h afterwards. The anovulatory women had comparable mean serum concentration of progesterone (0.9 +/- 0.5 nmol/L) to normal women and similar frequency of progesterone pulsatility (2.1 +/- 1.1 pulses/6 h). After administration of clomiphene, there was no significant change in progesterone pulsatility (1.7 +/- 1.0 pulses/6 h) despite a substantial increase in LH pulsatility (from none to 3.0 +/- 1.0 pulses/6 h). There was no significant increase in serum progesterone after clomiphene or GnRH which both caused a substantial increase in serum LH. The third study involved eight normal women studied before and after treatment with dexamethasone (2 mg/day for 2 days) to assess the adrenal component of progesterone secretion. Blood samples were collected every 10 min for 6 h before and 2 h after naloxone (5 mg iv). Dexamethasone reduced serum progesterone to below assay sensitivity (less than 0.2 nmol/L) and obliterated progesterone pulsatility. The increase in serum progesterone and cortisol induced by naloxone was blocked by dexamethasone; the naloxone-induced rise of serum LH was not affected by dexamethasone. We conclude that neither the preceding corpus luteum nor the developing follicle are important contributors to the serum concentration of progesterone during the normal follicular phase.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

本研究旨在确立正常月经周期卵泡期血清孕酮的正常模式及其分泌来源。在第一项研究中,12名正常女性在单个卵泡期的不同时间接受了3次研究。在注射纳洛酮(静脉注射5毫克)前6小时和注射后2小时内,每10分钟采集一次血清样本,共采集8小时。整个卵泡期血清孕酮均值保持恒定(0.9纳摩尔/升),直至排卵前;个体受试者显示孕酮有脉冲式分泌(1 - 6次脉冲/6小时),但这与促黄体生成素(LH)脉冲式分泌无关,且卵泡期内孕酮脉冲式分泌无变化。纳洛酮使卵泡早期血清孕酮均值升至1.9±0.7纳摩尔/升,卵泡中期和晚期分别升至2.1±0.7纳摩尔/升和3.4±2.5纳摩尔/升。第二项研究旨在评估残留黄体和发育中的卵泡对孕酮脉冲式分泌的贡献。对7名血清LH水平低且无LH脉冲式分泌的无排卵女性,在服用克罗米芬(100毫克/天,共5天)前后进行研究,在静脉注射促性腺激素释放激素(GnRH,10毫克)前6小时和注射后2小时内,每15分钟采集一次血样。这些无排卵女性的血清孕酮平均浓度(0.9±0.5纳摩尔/升)与正常女性相当,孕酮脉冲式分泌频率也相似(2.1±1.1次脉冲/6小时)。服用克罗米芬后,尽管LH脉冲式分泌大幅增加(从无到3.0±1.0次脉冲/6小时),但孕酮脉冲式分泌无显著变化(1.7±1.0次脉冲/6小时)。克罗米芬或GnRH均使血清LH大幅增加,但血清孕酮无显著升高。第三项研究涉及8名正常女性,在用地塞米松(2毫克/天,共2天)治疗前后进行研究,以评估孕酮分泌的肾上腺成分。在注射纳洛酮(静脉注射5毫克)前6小时和注射后2小时内,每10分钟采集一次血样。地塞米松使血清孕酮降至检测灵敏度以下(低于0.2纳摩尔/升),并消除了孕酮脉冲式分泌。地塞米松阻断了纳洛酮诱导的血清孕酮和皮质醇升高;纳洛酮诱导的血清LH升高不受地塞米松影响。我们得出结论,在正常卵泡期,前一个黄体和发育中的卵泡对血清孕酮浓度均无重要贡献。(摘要截选至400字)

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