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间歇性鼻内注射促黄体生成素释放激素激动剂联合口服孕激素作为抗排卵避孕方法的14天与21天方案

Fourteen-day versus twenty-one-day regimens of intermittent intranasal luteinizing hormone-releasing hormone agonist combined with an oral progestogen as antiovulatory contraceptive approach.

作者信息

Lemay A, Faure N

出版信息

J Clin Endocrinol Metab. 1986 Dec;63(6):1379-85. doi: 10.1210/jcem-63-6-1379.

Abstract

This study was designed to determine the effect of discontinuous administration of a LHRH agonist on pituitary-ovarian function in normal women. The LHRH agonist buserelin (200 micrograms/12 h or 400 micrograms/24 h) was given intranasally for four consecutive cycles for 14 or 21 days in 26 normally cycling women. Five milligrams of medroxyprogesterone acetate were given orally twice daily from days 15-21. There was a 7-day pause between each medication cycle. Blood samples were drawn every other day for RIA of LH, FSH, estradiol (E2), and progesterone (P). Serum FSH increased for only a few days at the beginning of each cycle, whereas sustained elevation of serum LH occurred during LHRH agonist administration. Serum E2 increased rapidly and remained elevated during the administration of buserelin. Serum P remained in the follicular phase range or increased briefly after the initiation of buserelin occasionally in the 14-day regimens. After discontinuation of buserelin, E2 fell rapidly, and uterine withdrawal bleeding occurred. During the pause, FSH increased progressively. The patterns of gonadotropin response to buserelin were similar in the four cycles. Based on measurement of the areas of the response curves, serum LH and E2 levels were higher during the administration of 200 micrograms/12 h compared to 400 micrograms/24 h buserelin. However, down-regulation of the pituitary-ovarian axis, as evaluated by the acute gonadotropin response to buserelin on day 14, was more pronounced with 200 micrograms/12 h than with 400 micrograms/24 h. Breakthrough bleeding occurred in the 14-day schedules, whereas withdrawal bleeding occurred during the pause in the 21-day schedules. The immediate cycles following buserelin administration were normal ovulatory cycles. Intermittent LHRH agonist administration for 21 days avoided constant down-regulation of the pituitary-ovarian axis and allowed regular uterine bleeding. Combined with an appropriate P complement, it could be a useful contraceptive approach.

摘要

本研究旨在确定间断给予促黄体生成激素释放激素(LHRH)激动剂对正常女性垂体 - 卵巢功能的影响。在26名月经周期正常的女性中,将LHRH激动剂布舍瑞林(200微克/12小时或400微克/24小时)经鼻内给药,连续四个周期,每次给药14天或21天。从第15至21天,每天口服两次5毫克醋酸甲羟孕酮。每个用药周期之间有7天的间歇期。每隔一天采集血样,用于放射免疫分析检测促黄体生成素(LH)、促卵泡生成素(FSH)、雌二醇(E2)和孕酮(P)。每个周期开始时血清FSH仅在几天内升高,而在给予LHRH激动剂期间血清LH持续升高。在布舍瑞林给药期间,血清E2迅速升高并持续维持在较高水平。在14天给药方案中,血清P维持在卵泡期水平,或在布舍瑞林开始给药后偶尔短暂升高。停用布舍瑞林后,E2迅速下降,并出现子宫撤退性出血。在间歇期,FSH逐渐升高。四个周期中促性腺激素对布舍瑞林的反应模式相似。根据反应曲线面积测量,与400微克/24小时布舍瑞林相比,在200微克/12小时布舍瑞林给药期间血清LH和E2水平更高。然而,在第14天通过急性促性腺激素对布舍瑞林的反应评估,200微克/12小时组垂体 - 卵巢轴的下调比400微克/24小时组更明显。在14天给药方案中出现突破性出血,而在21天给药方案的间歇期出现撤退性出血。布舍瑞林给药后的紧接着的周期为正常排卵周期。间断给予LHRH激动剂21天可避免垂体 - 卵巢轴持续下调,并使子宫有规律出血。结合适当的P补充剂,这可能是一种有用的避孕方法。

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