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大鼠促黄体素(黄体生成素)卵巢受体的研究。影响结合及反应的因素。

Studies on rat ovarian receptors for lutropin (luteinizing hormone). Factors influencing binding and response.

作者信息

Muralidhar K, Moudgal N R

出版信息

Biochem J. 1976 Dec 15;160(3):607-13. doi: 10.1042/bj1600607.

Abstract

The interaction of rat ovarian receptors with lutropin (luteinizing hormone, LH) in vitro was rapid and reversible. The degree of binding was saturable and susceptible to changes in the concentration of lutropin in the medium. The concentration of lutropin receptors in the ovary increases during the natural pubertal period and also in immature rats given pregnant-mare-serum gonadotropin and human choriogonadotropin. In the latter case, the increase in lutropin receptor, after injection of pregnant-mare-serum gonadotropin alone, could be detected only if the ovaries are freed of the bound gonadotropin before exposure to lutropin. The concentration of lutropin receptors was higher in the luteal compartment of the ovary than in the non-luteal parts and increased slightly in aged corpora lutea. Correlation between binding of lutropin to the ovary and the ovarian response to lutropin in terms of cyclic AMP production was found only in prepubertal rat ovaries and in young corpora lutea and not in aged corpora lutea, suggesting the non-equivalence of binding in vitro and ovarian response.

摘要

大鼠卵巢受体与促黄体激素(促性腺激素,LH)在体外的相互作用迅速且可逆。结合程度具有饱和性,并且易受培养基中促黄体激素浓度变化的影响。在自然青春期期间以及给予未成熟大鼠孕马血清促性腺激素和人绒毛膜促性腺激素时,卵巢中促黄体激素受体的浓度会增加。在后一种情况下,仅在将卵巢中的结合促性腺激素去除后再暴露于促黄体激素时,才能检测到单独注射孕马血清促性腺激素后促黄体激素受体的增加。卵巢黄体部分的促黄体激素受体浓度高于非黄体部分,并且在老化的黄体中略有增加。仅在青春期前大鼠卵巢和年轻黄体中发现促黄体激素与卵巢的结合与卵巢对促黄体激素在环磷酸腺苷产生方面的反应之间存在相关性,而在老化黄体中未发现,这表明体外结合与卵巢反应不等同。

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本文引用的文献

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Steroid A-Ring reduction by rat ovaries.大鼠卵巢对甾体A环的还原作用。
Endocrinology. 1970 Aug;87(2):350-5. doi: 10.1210/endo-87-2-350.
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Gonadotropins, ovarian metabolism, and steroid biosynthesis.促性腺激素、卵巢代谢与类固醇生物合成
Recent Prog Horm Res. 1968;24:255-319. doi: 10.1016/b978-1-4831-9827-9.50012-5.
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Characteristics of gonadotropin receptors of porcine granulosa cells during follicle maturation.
Endocrinology. 1973 Feb;92(2):531-40. doi: 10.1210/endo-92-2-531.

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