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抗孕激素抑制由7,12-二甲基苯并(a)蒽诱导的已建立肿瘤的生长:RU486与一种新的21-取代-19-去甲孕激素的比较。

Anti-progestins suppress the growth of established tumors induced by 7,12-dimethylbenz(a)anthracene: comparison between RU486 and a new 21-substituted-19-nor-progestin.

作者信息

Wiehle Ronald D, Christov Konstantin, Mehta Rajendra

机构信息

Repros Therapeutics Inc., The Woodlands, TX 77380, USA.

出版信息

Oncol Rep. 2007 Jul;18(1):167-74.

Abstract

In this report, we evaluate the effects of a 21-substituted-19-nor-progestin, CDB-4124, on 7,12,-dimethylbenz(a)anthracene (DMBA)-induced mammary carcinogenesis in rats in comparison with RU486. Sprague-Dawley female rats were treated with DMBA at 50 days of age in order to induce mammary tumors. When the tumors reached the size of 10-12 mm, the animals were treated for 28 days with the vehicle, RU486, progesterone, CDB-4124 at various doses, or CDB-4124 plus progesterone. Anti-progestins resulted in the regression in the size of the existing tumors, and in the suppressed development of new tumors and tumor multiplicity. Progesterone treatment, however, increased the size and multiplicity. Progesterone rendered an increased number of growing tumors as compared to the regression in the anti-progesterone treatment groups. The combination of CDB-4124 and high doses of progesterone opposed the efficacy of CDB-4124. The growth inhibitory effects of the anti-progestins were correlated with increased apoptosis and reduced cell proliferation. These results indicate that anti-progestins should be developed for the chemoprevention and treatment of hormone-responsive breast cancer.

摘要

在本报告中,我们评估了一种21-取代-19-去甲孕酮CDB-4124与RU486相比,对7,12-二甲基苯并(a)蒽(DMBA)诱导的大鼠乳腺癌发生的影响。在50日龄时用DMBA处理斯普拉格-道利雌性大鼠以诱导乳腺肿瘤。当肿瘤长到10-12毫米大小时,用赋形剂、RU486、孕酮、不同剂量的CDB-4124或CDB-4124加孕酮对动物进行28天的治疗。抗孕激素导致现有肿瘤体积缩小,并抑制新肿瘤的发生和肿瘤的多样性。然而,孕酮治疗会增加肿瘤的大小和多样性。与抗孕激素治疗组肿瘤的消退相比,孕酮使生长中的肿瘤数量增加。CDB-4124与高剂量孕酮联合使用会对抗CDB-4124的疗效。抗孕激素的生长抑制作用与细胞凋亡增加和细胞增殖减少相关。这些结果表明,抗孕激素应被开发用于激素反应性乳腺癌的化学预防和治疗。

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