子宫内膜形态和出血模式作为孕激素补充的功能。

D W Sturdee
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引用次数: 0

摘要

绝经后妇女在雌激素替代疗法中加入孕激素,以预防子宫内膜增生和腺癌,并在序贯疗法中促进规律和可预测的出血。孕激素的这种保护作用是公认的,但它不是由于子宫内膜脱落在隐退性出血,不能从出血的模式或时间预测。虽然不规则出血可能是子宫内膜异常和孕激素不足的反映,但子宫内膜异常也可能发生有规律的可控出血。一项针对绝经后妇女的大型多中心研究发现,服用标准28天序贯雌激素和孕激素方案的妇女出现了2.7%的复杂增生,其中大多数妇女有正常和规律的出血模式。萎缩的子宫内膜也可能出现常规出血。采用较长周期的治疗,每4个月或4个月给予一次孕激素,可以提高患者长期治疗的持续性。在单雌激素期,子宫内膜逐渐增生,约12周后可出现单纯性或囊性增生,可通过孕激素纠正。尽管突破性出血的发生率比每月出血的发生率高,但女性似乎更喜欢不太频繁的退缩性出血。每天服用雌激素和孕激素的持续联合治疗不会导致退缩性出血,尽管有些人在最初的2或3个月会有轻微的突破性出血。持续的孕激素治疗使子宫内膜萎缩,并将序贯治疗期间发生的已存在的复杂子宫内膜增生转化为正常状态。到目前为止,还没有临床指南可以保证绝经后接受激素替代疗法的妇女子宫内膜的状态。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Endometrial morphology and bleeding patterns as a function of progestogen supplementation.

Progestogens are added to estrogen replacement therapy for postmenopausal women to prevent endometrial hyperplasia and adenocarcinoma, and in sequential therapy to promote a regular and predictable bleed. This protective effect of progestogens is well recognized, but it is not due to endometrial shedding at a withdrawal bleed and cannot be predicted from the pattern or timing of the bleed. While irregular bleeding may be a reflection of endometrial abnormality and possibly insufficient progestogen, a regular controlled bleed may also occur in the presence of endometrial abnormality. A large multicenter study of postmenopausal women who were taking standard 28-day sequential regimens of estrogen and progestogen found a 2.7% prevalence of complex hyperplasia, and most of these women had a normal and regular bleeding pattern. Regular bleeding may also occur from an atrophic endometrium. Therapy employing a longer cycle with a course of progestogen given every 4 or 4 months may improve patient continuance for long-term therapy. During the estrogen-only phase, the endometrium becomes increasingly proliferative, and simple or cystic hyperplasia may develop only after about 12 weeks, and then can be corrected by progestogen. Women seem to prefer a less frequent withdrawal bleed despite the higher incidence of breakthrough bleeding compared to a monthly loss. Continuous combined therapy with estrogen and progestogen taken every day causes no withdrawal bleed, though some will have light breakthrough bleeding for the initial 2 or 3 months. The continuous progestogen keeps the endometrium atrophic and also converts preexisting complex endometrial hyperplasia occurring during sequential therapy to a normal state. As yet, there are no clinical guidelines that can give reassurance about the state of the endometrium in postmenopausal women who are taking hormone replacement therapy.

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