Bakker G H, Setyono-Han B, Henkelman M S, de Jong F H, Lamberts S W, van der Schoot P, Klijn J G
Department of Endocrine Oncology, Dr. Daniel den Hoed Cancer Center, Rotterdam, The Netherlands.
Cancer Treat Rep. 1987 Nov;71(11):1021-7.
The effects of the synthetic antiprogestin mifepristone (RU486) on growth of dimethylbenzanthracene (DMBA)-induced mammary tumors in female rats were investigated. Prophylactic treatment with mifepristone (10 mg/kg/day) for 3 weeks starting from the day of first DMBA injection resulted in a doubling of the average tumor latency period (81 +/- 16 days, n = 17 treated, versus 39 +/- 5 days, n = 75 controls; P less than 0.005) and was accompanied by a significant growth retardation as shown by lower body weight increments. A 3-week therapeutic treatment of rats bearing mammary tumors was performed by administration of different dosages of mifepristone (2.5, 10, or 40 mg/kg/day) or megestrol acetate (2.5 or 10 mg/kg/day), with the luteinizing hormone-releasing hormone agonist buserelin (40 micrograms/kg/day), buserelin plus mifepristone (10 mg/kg/day), or by ovariectomy. The effects of treatment on tumor load, pituitary, adrenal and reproductive organ weights, steroid receptor contents of mammary tumors, and blood plasma hormone concentrations were investigated. Mifepristone and megestrol acetate treatment gave rise to inhibition of mammary tumor growth with all dosages studied, in which mifepristone was more potent than megestrol acetate (80%-90% vs 40% inhibition, P less than 0.01). In contrast, buserelin treatment and ovariectomy resulted not only in inhibition, but in tumor remission by about 50%. Combined treatment with buserelin and mifepristone gave the same tumor remission as resulted from ovariectomy or single treatment with buserelin. Estradiol-stimulated growth of the human mammary cancer MCF-7 cells in culture was fully abolished by mifepristone (3.6 X 10(-8) M) or tamoxifen (4 X 10(-8) M), whereas growth of MCF-7 cells under control incubation was not affected by either agent. Therefore, a direct inhibition of the growth of rat mammary tumor cells by mifepristone appears likely. Based on the effects of mifepristone on plasma hormone levels (increased: luteinizing hormone, estradiol, progesterone; unchanged: follicle-stimulating hormone, adrenocorticotropic hormone, corticosterone), organ weights (increased: pituitary, ovaries, uterus; unchanged: adrenals) and steroid receptor contents of mammary tumors (decreased: estrogen receptor and progesterone receptor contents), the main mechanism of action is probably a direct antiprogestational effect at the level of the mammary tumor cells through occupancy of the progesterone receptor.
研究了合成抗孕激素米非司酮(RU486)对雌性大鼠二甲基苯并蒽(DMBA)诱导的乳腺肿瘤生长的影响。从首次注射DMBA之日起,用米非司酮(10毫克/千克/天)进行预防性治疗3周,导致平均肿瘤潜伏期加倍(治疗组17只,81±16天,对照组75只,39±5天;P<0.005),并伴有体重增加明显减缓。对患有乳腺肿瘤的大鼠进行为期3周的治疗,给予不同剂量的米非司酮(2.5、10或40毫克/千克/天)或醋酸甲地孕酮(2.5或10毫克/千克/天),同时给予促黄体生成素释放激素激动剂布舍瑞林(40微克/千克/天)、布舍瑞林加米非司酮(10毫克/千克/天),或进行卵巢切除术。研究了治疗对肿瘤负荷、垂体、肾上腺和生殖器官重量、乳腺肿瘤的类固醇受体含量以及血浆激素浓度的影响。米非司酮和醋酸甲地孕酮治疗在所研究的所有剂量下均能抑制乳腺肿瘤生长,其中米非司酮比醋酸甲地孕酮更有效(抑制率80% - 90% vs 40%,P<0.01)。相比之下,布舍瑞林治疗和卵巢切除术不仅能抑制肿瘤,还能使肿瘤缓解约50%。布舍瑞林和米非司酮联合治疗产生的肿瘤缓解效果与卵巢切除术或单独使用布舍瑞林治疗相同。米非司酮(3.6×10⁻⁸M)或他莫昔芬(4×10⁻⁸M)能完全消除培养的人乳腺癌MCF - 7细胞在雌二醇刺激下的生长,而在对照培养条件下,MCF - 7细胞的生长不受这两种药物的影响。因此,米非司酮似乎可能直接抑制大鼠乳腺肿瘤细胞的生长。基于米非司酮对血浆激素水平(升高:促黄体生成素、雌二醇、孕酮;不变:促卵泡激素、促肾上腺皮质激素、皮质酮)、器官重量(增加:垂体、卵巢、子宫;不变:肾上腺)以及乳腺肿瘤的类固醇受体含量(降低:雌激素受体和孕酮受体含量)的影响,其主要作用机制可能是通过占据孕酮受体,在乳腺肿瘤细胞水平产生直接的抗孕激素作用。
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