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雌二醇刺激无胸腺小鼠体内植入的MCF-7肿瘤生长:一种研究他莫昔芬抑瘤作用的模型。

Estradiol-stimulated growth of MCF-7 tumors implanted in athymic mice: a model to study the tumoristatic action of tamoxifen.

作者信息

Gottardis M M, Robinson S P, Jordan V C

机构信息

Department of Human Oncology, University of Wisconsin Clinical Cancer Center, Madison 53792.

出版信息

J Steroid Biochem. 1988;30(1-6):311-4. doi: 10.1016/0022-4731(88)90113-6.

Abstract

Ovariectomized athymic (nude) mice were inoculated (10(7) cells) with the breast cancer cell line, MCF-7, into the axillary mammary fat pads. Tumors did not grow unless animals were implanted with a 1.7 mg estradiol sustained (8-week)-release cholesterol pellet. Co-implantation with tamoxifen (5 mg, 4-week release) caused an inhibition of estradiol-stimulated growth but did not cause tumor growth when implanted alone. The metabolism of [3H]tamoxifen was determined in the athymic mouse bearing MCF-7 tumors. Metabolites in the liver, uterus and tumor were determined by TLC. The principal metabolite in each of the tissues was 4-hydroxytamoxifen (by comparison of Rfs with authentic standards). Studies with 4-hydroxytamoxifen and N-desmethyltamoxifen (the principal metabolites in patients) showed that each was effective in inhibiting estradiol-stimulated tumor growth. However, tumor growth could be reactivated by treatment with estradiol alone. In a separate experiment, tumor-implanted animals were treated with tamoxifen for 1, 2 and 6 months. Tamoxifen did not cause tumor growth. Nevertheless, tumor growth was reactivated by estradiol on each occasion. These studies confirm the tumoristatic actions of tamoxifen and strongly support the view that therapy must be given indefinitely to patients to control tumor recurrence. The athymic mouse model can be used in the future to determine the efficacy of novel antiestrogens and the development of antiestrogen drug resistance.

摘要

将切除卵巢的无胸腺(裸)小鼠在腋窝乳腺脂肪垫接种(10⁷个细胞)乳腺癌细胞系MCF - 7。除非给动物植入1.7毫克雌二醇缓释(8周)胆固醇丸剂,肿瘤不会生长。与他莫昔芬(5毫克,4周释放)共同植入会抑制雌二醇刺激的生长,但单独植入时不会导致肿瘤生长。在携带MCF - 7肿瘤的无胸腺小鼠中测定了[³H]他莫昔芬的代谢情况。通过薄层层析法测定肝脏、子宫和肿瘤中的代谢产物。每个组织中的主要代谢产物都是4 - 羟基他莫昔芬(通过与标准品比较Rf值)。对4 - 羟基他莫昔芬和N - 去甲基他莫昔芬(患者中的主要代谢产物)的研究表明,每种物质都能有效抑制雌二醇刺激的肿瘤生长。然而,单独用雌二醇治疗可使肿瘤生长重新激活。在另一项实验中,给植入肿瘤的动物用他莫昔芬治疗1、2和6个月。他莫昔芬不会导致肿瘤生长。尽管如此,每次雌二醇都能使肿瘤生长重新激活。这些研究证实了他莫昔芬的抑瘤作用,并有力地支持了必须对患者进行无限期治疗以控制肿瘤复发的观点。未来可利用无胸腺小鼠模型来确定新型抗雌激素药物的疗效以及抗雌激素耐药性的发展情况。

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