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7,12-二甲基苯并(a)蒽诱导的肿瘤中的雌激素-催乳素依赖性

Estrogen-prolactin dependency in 7,12-dimethylbenz(a)anthracene-induced tumors.

作者信息

Leung B S, Sasaki G H, Leung J S

出版信息

Cancer Res. 1975 Mar;35(3):621-7.

PMID:163687
Abstract

Hormonal influences on dimethylbenz(a)anthracene-induced tumor growth were investigated in detail by endocrine ablation and replacement of hormones. The majority of tumors regressed following ablation and most of them were reactivated by subsequent administrations of estrogen (0.1 to 5 mug) or prolactin (2 mg). Increasing numbers of tumors, however, were not stimulated by prolactin when administration was delayed, and a basal level of estradiol (0.01 mug) in addition to prolactin was required for reactivation of tumors. Nafoxidine hydrochloride, a competitor of estrogen at the receptor sites, arrested growth of a large portion of dimethylbenz(a)anthracene-induced tumors in intact animals but failed to retard growth of prolactin-stimulated tumors. On withdrawal of prolactin-nafoxidine, rapid regression of tumor occurred and readministration of prolactin failed to activate most of the tumors for as long as 28 days. Our results give good supporting evidence that estrogen plays a primary role in tumor growth. The interactions of prolactin and estrogen at tumor sites are necessary for regulatory events related to tumor growth.

摘要

通过内分泌切除和激素替代,详细研究了激素对二甲基苯并(a)蒽诱导的肿瘤生长的影响。大部分肿瘤在切除后消退,其中大多数在随后给予雌激素(0.1至5微克)或催乳素(2毫克)后重新激活。然而,当给药延迟时,越来越多的肿瘤不受催乳素刺激,并且除催乳素外,还需要基础水平的雌二醇(0.01微克)来重新激活肿瘤。盐酸萘福昔定是雌激素在受体部位的竞争者,它能阻止完整动物中大部分二甲基苯并(a)蒽诱导的肿瘤生长,但不能抑制催乳素刺激的肿瘤生长。停用催乳素-萘福昔定后,肿瘤迅速消退,再次给予催乳素在长达28天的时间内未能激活大多数肿瘤。我们的结果提供了有力的支持证据,表明雌激素在肿瘤生长中起主要作用。催乳素和雌激素在肿瘤部位的相互作用对于与肿瘤生长相关的调节事件是必要的。

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