孕酮、睾酮及合成孕激素对生长因子和雌二醇处理的人乳腺癌及良性乳腺细胞的影响。
The effect of progesterone, testosterone and synthetic progestogens on growth factor- and estradiol-treated human cancerous and benign breast cells.
作者信息
Krämer Elizabeth A, Seeger Harald, Krämer Bernhard, Wallwiener Diethelm, Mueck Alfred O
机构信息
Section of Endocrinology and Menopause, University Women's Hospital, Calwerstrasse 7, 72 076 Tuebingen, Germany.
出版信息
Eur J Obstet Gynecol Reprod Biol. 2006 Nov;129(1):77-83. doi: 10.1016/j.ejogrb.2005.12.004. Epub 2006 Feb 7.
OBJECTIVE
The effects of progesterone (P), testosterone (T), chlormadinone acetate (CMA), medroxyprogesterone acetate (MPA), norethisterone (NET), levonorgestrel (LNG), dienogest (DNG), gestodene (GSD) and 3-ketodesogestrel (KDG) were investigated in normal human breast epithelial MCF10A cells. In addition, the effects of these steroids were tested in estrogen and progesterone receptor positive HCC1500 human primary breast cancer cells.
STUDY DESIGN
MCF10A cells were incubated with each progestogen at 1 microM and 100 nM for 7 days with growth factors epidermal growth factor (EGF), fibroblast growth factor (FGF) and insulin-like growth factor (IGF-I) (GFs, each 1 pM), and HCC1500 cells with GFs and/or estradiol (E2) 100 pM. Cell proliferation rate was measured by ATP-assay and cell death by photometric enzyme immunoassay. Ratios of cell death:proliferation were calculated.
RESULTS
MPA and CMA with GFs induced proliferation of MCF10A cells. P, T, NET, LNG, DNG, GSD and KDG had no significant effect. In HCC1500 cells, MPA and CMA with GFs had an inhibitory effect compared to GFs alone. NET, LNG, DNG, GSD, KDG and T enhanced the proliferative effect of GFs. P had no significant effect. No progestogen could further enhance the stimulatory effect of E2 on HCC1500 cells; all but KDG inhibited it. MPA, GSD, T, CMA and NET had an anti-proliferative effect on the mitotic GF and E2 combination. P, LNG, DNG and KDG had no significant effect.
CONCLUSIONS
Estrogens and mitogenic growth factors from stromal breast tissue are significant in growth-regulation of breast cells and may alter responses to progestogens. Certain progestogens are able to induce proliferation of or inhibit growth of benign or malignant human breast epithelial cells independently of the effects of growth factors and E2; therefore, choice of progestogen for hormone therapy may be important in terms of influencing possible breast cancer risk.
目的
研究孕酮(P)、睾酮(T)、醋酸氯地孕酮(CMA)、醋酸甲羟孕酮(MPA)、炔诺酮(NET)、左炔诺孕酮(LNG)、地诺孕素(DNG)、孕二烯酮(GSD)和3-酮去氧孕烯(KDG)对正常人类乳腺上皮MCF10A细胞的影响。此外,还检测了这些甾体激素对雌激素和孕激素受体阳性的HCC1500人原发性乳腺癌细胞的影响。
研究设计
将MCF10A细胞与每种孕激素分别在1μM和100 nM浓度下孵育7天,同时加入表皮生长因子(EGF)、成纤维细胞生长因子(FGF)和胰岛素样生长因子(IGF-I)(每种生长因子浓度均为1 pM);将HCC1500细胞与生长因子和/或100 pM雌二醇(E2)孵育。通过ATP检测法测量细胞增殖率,通过光度酶免疫测定法检测细胞死亡情况。计算细胞死亡与增殖的比率。
结果
MPA和CMA与生长因子共同作用可诱导MCF10A细胞增殖。P、T、NET、LNG、DNG、GSD和KDG无显著作用。在HCC1500细胞中,与单独使用生长因子相比,MPA和CMA与生长因子共同作用具有抑制作用。NET、LNG、DNG、GSD、KDG和T增强了生长因子的增殖作用。P无显著作用。没有一种孕激素能进一步增强E2对HCC1500细胞的刺激作用;除KDG外,所有孕激素均抑制该作用。MPA、GSD、T、CMA和NET对有丝分裂生长因子和E2的联合作用具有抗增殖作用。P、LNG、DNG和KDG无显著作用。
结论
来自乳腺基质组织的雌激素和有丝分裂生长因子在乳腺细胞的生长调节中起重要作用,可能会改变对孕激素的反应。某些孕激素能够独立于生长因子和E2的作用,诱导良性或恶性人类乳腺上皮细胞增殖或抑制其生长;因此,就影响潜在乳腺癌风险而言,激素治疗中孕激素的选择可能很重要。
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