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各种孕酮类似物的糖皮质激素活性:胸腺和肝脏中的特异性结合与生物活性之间的相关性。

Glucocorticoid activity of various progesterone analogs: correlation between specific binding in thymus and liver and biologic activity.

作者信息

DiSorbo D, Rosen F, McPartland R P, Milholland R J

出版信息

Ann N Y Acad Sci. 1977 Mar 11;286:355-68. doi: 10.1111/j.1749-6632.1977.tb29429.x.

Abstract

When tested in an in vitro assay system, progesterone and various analogs of this steroid were shown to compete with [3H] triamcinolone acetonide (TA) for specific glucocorticoid receptors in both rat liver and thymus. Of these analogs, the following derivatives of progesterone were potent competitors of TA binding and, when injected into adrenalectomized rats, induced regression of the thymus and marked increases in hepatic tyrosine aminotransferase activity: 11 beta-hydroxyl, 6 alpha-methyl, 6 alpha, 16 alpha-dimethyl, and 6 alpha-methyl-17 alpha-hydroxyl. In contrast, progesterone, 16 alpha-methyl, and 17 alpha-hydroxy progesterone competed with TA in vitro but failed to elicit either gluco- or antiglucocorticoid activity in vivo. Also, we observed that the oral contraceptive 6 alpha-methyl-17-(1-propynyl)testosterone competes very effectively with TA in a cell-free preparation of rat liver and induces an increase in hepatic tyrosine aminotransferase activity. The 11 beta-hydroxyl group has previously been thought to be essential for glucocorticoid activity. Our studies indicate that substitution of progesterone or testosterone with a 6 alpha-methyl group negates the need for an 11 beta-hydroxyl substitutuent as a prerequisite for glucocorticoid activity.

摘要

在体外分析系统中进行测试时,孕酮及其各种甾体类似物被证明能与[3H]曲安奈德(TA)竞争大鼠肝脏和胸腺中的特异性糖皮质激素受体。在这些类似物中,以下孕酮衍生物是TA结合的有效竞争者,当注射到肾上腺切除的大鼠体内时,会导致胸腺萎缩并使肝脏酪氨酸转氨酶活性显著增加:11β-羟基、6α-甲基、6α,16α-二甲基和6α-甲基-17α-羟基。相比之下,孕酮、16α-甲基和17α-羟基孕酮在体外能与TA竞争,但在体内未能引发糖皮质激素或抗糖皮质激素活性。此外,我们观察到口服避孕药6α-甲基-17-(1-丙炔基)睾酮在大鼠肝脏的无细胞制剂中能非常有效地与TA竞争,并能使肝脏酪氨酸转氨酶活性增加。11β-羟基基团以前被认为是糖皮质激素活性所必需的。我们的研究表明,用6α-甲基取代孕酮或睾酮可消除将11β-羟基取代基作为糖皮质激素活性前提条件的必要性。

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