染料木素对大鼠子宫和阴道中转化生长因子- α、表皮生长因子(EGF)及EGF受体表达的调控。

N M Brown, C A Lamartiniere
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引用次数: 0

摘要

流行病学报告和实验室数据表明大豆和染料木素与降低子宫癌、乳腺癌和前列腺癌、心血管疾病和骨质疏松症的发病率以及降低总血胆固醇有关。本研究旨在探讨染料木素在大鼠子宫和阴道中的作用,重点关注转化生长因子(TGF) α、表皮生长因子(EGF)及其受体的分布。产后16、18、20天给大鼠注射染料木黄酮(500微克/克体重),可导致子宫湿增重,21日龄大鼠子宫管腔上皮、腺上皮和阴道鳞状上皮增生。50日龄时,子宫和阴道不再明显肥大。青春期前染料木黄酮治疗导致个体间质细胞中EGF免疫染色显著增加,子宫血管中EGF受体免疫染色显著降低。染料木黄酮处理大鼠子宫腺上皮和腔上皮的tgf - α免疫染色降低,基质细胞的EGF受体免疫染色略有增加。这表明细胞间的旁分泌相互作用提高了基质中EGF配体和管腔上皮和腺上皮中EGF受体的水平,导致子宫肥大。在21日龄和50日龄大鼠的阴道中,染料木素没有引起egf信号通路的显著改变。我们得出结论,在青春期前服用染料木素可以调节子宫内的egf信号通路,并在短期内产生子宫营养反应。
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Genistein regulation of transforming growth factor-alpha, epidermal growth factor (EGF), and EGF receptor expression in the rat uterus and vagina.

Epidemiological reports and laboratory data have associated soy and genistein with reduced incidence of uterine, breast, and prostate cancers, cardiovascular disease and osteoporosis, and lower total blood cholesterol. The aim of this study was to investigate the effect of genistein in the uterus and vagina of rats, focusing our attention on the distribution of transforming growth factor (TGF) alpha, epidermal growth factor (EGF), and EGF receptor. A pharmacological dose of genistein (500 microg/g body weight) injected in rats on days 16,18, and 20 postpartum resulted in significant uterine wet weight gain, with hypertrophy of the luminal and glandular epithelium of the uteri, and squamous epithelium of the vagina in 21-day-old animals. At 50 days of age, hypertrophy was no longer evident in the uterus and vagina. Prepubertal genistein treatment resulted in significantly increased EGF immunostaining in individual stromal cells and reduced EGF receptor immunostaining in blood vessels of the uterus. Genistein-treated rats had decreased TGF-alpha immunostaining in glandular and luminal epithelium and a slight increase in EGF receptor immunostaining in stromal cells of the uterus. This suggests paracrine interaction between cells elevating the level of EGF ligand in the stroma and the EGF receptor in the luminal and glandular epithelium, resulting in uterine hypertrophy. In the vagina, genistein did not cause significant alterations to the EGF-signaling pathway in 21- and 50-day-old rats. We conclude that pharmacological doses of genistein during the prepubertal period can modulate the EGF-signaling pathway in the uterus and exert a uterotrophic response in a short-term manner.

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