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体外超灌注大鼠下丘脑释放促黄体生成激素:孕酮的作用位点及雌激素预处理的影响

In vitro luteinizing hormone-releasing hormone release from superfused rat hypothalami: site of action of progesterone and effect of estrogen priming.

作者信息

Kim K, Ramirez V D

出版信息

Endocrinology. 1985 Jan;116(1):252-8. doi: 10.1210/endo-116-1-252.

Abstract

The study examined the effect of estrogen priming on progesterone (P4)-induced LHRH release, the tissue site of action of P4, and the effect of 5 alpha-dihydroxyprogesterone (5 alpha-DHP) on LHRH release from hypothalamic fragments superfused in vitro. Immature female rats were ovariectomized (OVX) and, at 28 days of age, Silastic capsules containing estradiol (E2) were implanted. Two days later, animals were killed and hypothalamic fragments were removed and transferred to superfusion chambers. The hypothalamic units received P4 or 5 alpha-DHP delivered in an intermittent mode (10-min on, 20-min off). LHRH was determined in perfusates by RIA. After the input characteristics of different infusion modes (single pulses, intermittent, and continuous) of P4 infused into superfusion chambers were assessed, an intermittent infusion mode (10-min on, 20-min off) was selected for further examinations. In the mediobasal hypothalamic-anterior hypothalamic-preoptic area (MBH-AHA-POA) tissue preparations, we observed: 1) an infusion of 5 alpha-DHP was ineffective in stimulating LHRH release; 2) the release pattern of LHRH in response to three different P4 doses (10, 20, and 50 ng/ml) was similar in terms of percent changes (202% to 219% over control values); and 3) E2 priming was absolutely required for P4-stimulated LHRH release, and this requirement appeared to be dose dependent. Upon an examination of three hypothalamic tissue boundaries [the MBH, the POA-suprachiasmatic nuclei (POA-SCN), and the median eminence (ME)] to better delineate the in vitro site of action of P4 on LHRH release, it was demonstrated that the MBH responded upon P4 infusion, whereas the POA-SCN was unable to do so. The ME also responded upon P4 infusion, and LHRH release followed closely the pulsatile administration of P4 since upon each challenge of the steroid at the concentration of 10 or 20 ng/ml, a significant rise in LHRH release occurred. However, the temporal patterns of LHRH release from the ME appears to be different from those obtained from the MBH as well as the MBH-AHA-POA. These observations demonstrate that an intermittent infusion of P4, but not 5 alpha-DHP, is effective in activating the neural LHRH apparatus. Estrogen is an obligatory requirement for this P4-stimulated LHRH release, and the neural site of action of P4 resides within the MBH. However, this steroid also can act directly upon the ME nerve terminals to release LHRH.

摘要

该研究考察了雌激素预处理对孕酮(P4)诱导的促性腺激素释放激素(LHRH)释放的影响、P4的组织作用位点以及5α-二羟孕酮(5α-DHP)对体外灌流的下丘脑片段释放LHRH的影响。将未成年雌性大鼠进行卵巢切除(OVX),并在28日龄时植入含雌二醇(E2)的硅橡胶胶囊。两天后,处死动物,取出下丘脑片段并转移至灌流室。下丘脑单位接受以间歇模式(开10分钟,关20分钟)给予的P4或5α-DHP。通过放射免疫分析法(RIA)测定灌流液中的LHRH。在评估了注入灌流室的P4的不同输注模式(单脉冲、间歇和连续)的输入特性后,选择了间歇输注模式(开10分钟,关20分钟)进行进一步研究。在中基底下丘脑-前下丘脑-视前区(MBH-AHA-POA)组织制备中,我们观察到:1)注入5α-DHP对刺激LHRH释放无效;2)LHRH对三种不同P4剂量(10、20和50 ng/ml)的释放模式在变化百分比方面相似(比对照值高202%至219%);3)E2预处理是P4刺激LHRH释放的绝对必要条件,且这种需求似乎呈剂量依赖性。在检查三个下丘脑组织边界[MBH、视前区-视交叉上核(POA-SCN)和正中隆起(ME)]以更好地确定P4对LHRH释放的体外作用位点时,发现注入P4后MBH有反应,而POA-SCN无反应。注入P4后ME也有反应,且LHRH释放紧密跟随P4的脉冲给药,因为在以10或20 ng/ml浓度每次给予该类固醇时,LHRH释放会显著增加。然而,ME释放LHRH的时间模式似乎与从MBH以及MBH-AHA-POA获得的数据不同。这些观察结果表明,间歇注入P4而非5α-DHP可有效激活神经LHRH装置。雌激素是这种P4刺激的LHRH释放的必要条件,且P4的神经作用位点位于MBH内。然而,这种类固醇也可直接作用于ME神经末梢以释放LHRH。

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