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孕酮拮抗剂的抗排卵潜力与下丘脑、垂体和卵巢中孕酮受体的下调相关。

The antiovulatory potential of progesterone antagonists correlates with a down-regulation of progesterone receptors in the hypothalamus, pituitary and ovaries.

作者信息

Donath J, Nishino Y, Schulz T, Michna H

机构信息

Department of Morphology and Tumor Research, DSHS, Cologne, Germany.

出版信息

Ann Anat. 2000 Mar;182(2):143-50. doi: 10.1016/S0940-9602(00)80073-4.

Abstract

These studies analyze the regulation of progesterone receptors (PRs) in central and peripheral tissues with the aim of further understanding mechanistically the inhibition of ovulation by progesterone antagonists (PA). Therefore, it was of interest to investigate the influence of the progesterone receptor antagonist, Onapristone (ON), on PRs in the ovary, pituitary (PT), and hypothalamus (HYP), since ON effectively inhibits ovulation in rats. For this study PMSG/hCG-primed immature and adult female rats were treated with ON. Immunohistochemistry was used for the detection of PRs. Progesterone (P4) and estradiol (E2) levels were determined by RIA. PR expression in the ovaries of immature rats was not detectable until after hCG administration. In these animals, ON caused a reduction in the staining intensity of PR in the tertiary follicles at the time when the preovulatory P4-surge was inhibited (6 h post hCG). Adult rats treated for 15 days with ON showed a decreased PR expression in PT and HYP. At this time (proestrus, 7 p.m.) the P4 and E2 levels are significantly lowered. These results suggest that after treatment with ON the expression of PR is reduced in the ovary, PT and HYP. The regulation of PR in the ovary seems to be less dependent on estrogens than on LH. Thus, it is conceivable that the reduced PR expression after ON treatment may be a result of decreased LH sensitivity in the ovary. In the pituitary and hypothalamus, PR expression is stimulated by estrogens and progesterone, and therefore the fall in the P4 and E2 levels in ON-treated animals may be responsible for the reduced PR expression in PT and HYP, and may contribute to the antiovulatory effect of ON. We therefore conclude that the mechanism of the antiovulatory potency of progesterone antagonists is based on a reduced preovulatory P4-production and PR expression in the ovary and also on the down-regulation of PR in the anterior pituitary and hypothalamus.

摘要

这些研究分析了中枢和外周组织中孕酮受体(PRs)的调节情况,目的是从机制上进一步了解孕酮拮抗剂(PA)对排卵的抑制作用。因此,研究孕酮受体拮抗剂奥那司酮(ON)对卵巢、垂体(PT)和下丘脑(HYP)中PRs的影响很有意义,因为ON能有效抑制大鼠排卵。在本研究中,用PMSG/hCG预处理的未成熟和成年雌性大鼠接受了ON治疗。采用免疫组织化学法检测PRs。通过放射免疫分析法测定孕酮(P4)和雌二醇(E2)水平。未成熟大鼠直到注射hCG后才能检测到卵巢中的PR表达。在这些动物中,当排卵前P4高峰被抑制时(hCG注射后6小时),ON导致三级卵泡中PR的染色强度降低。用ON处理15天的成年大鼠在PT和HYP中的PR表达降低。此时(发情前期,晚上7点),P4和E2水平显著降低。这些结果表明,用ON治疗后,卵巢、PT和HYP中PR的表达降低。卵巢中PR的调节似乎对雌激素的依赖性小于对促黄体生成素(LH)的依赖性。因此,可以想象,ON治疗后PR表达降低可能是卵巢中LH敏感性降低的结果。在垂体和下丘脑中,PR表达受到雌激素和孕酮的刺激,因此,ON处理动物中P4和E2水平的下降可能是PT和HYP中PR表达降低的原因,并且可能有助于ON的抗排卵作用。因此,我们得出结论,孕酮拮抗剂抗排卵作用的机制是基于排卵前卵巢中P4产生和PR表达的减少,以及垂体前叶和下丘脑中PR的下调。

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