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异雌激素双酚A可诱导雌性生殖道的生长、分化及c-fos基因表达。

The xenoestrogen bisphenol A induces growth, differentiation, and c-fos gene expression in the female reproductive tract.

作者信息

Steinmetz R, Mitchner N A, Grant A, Allen D L, Bigsby R M, Ben-Jonathan N

机构信息

Department of Obstetrics and Gynecology, Indiana University School of Medicine, Indianapolis 46202, USA.

出版信息

Endocrinology. 1998 Jun;139(6):2741-7. doi: 10.1210/endo.139.6.6027.

Abstract

The xenoestrogen bisphenol A (BPA) has been shown to mimic estrogen both in vivo and in vitro. BPA stimulates PRL secretion and the expression of a PRL regulating factor from the posterior pituitary in the estrogen-sensitive Fischer 344 rat (F344), but not in Sprague-Dawley (SD) rats. The goal of the present studies was to examine the in vivo actions of BPA on the reproductive tract. The specific objectives were 1) to characterize the short term effects of BPA on cell proliferation and c-fos expression in the uterus and vagina, and 2) to compare the effects of prolonged exposure to low doses of BPA on the reproductive tract of F344 and SD rats. Treatment with single high doses of BPA induced cell proliferation in the uterus and vagina of ovariectomized F344 rats, as determined by bromodeoxyuridine immunostaining. This proliferation was dose dependent (from 37.5-150 mg/kg) and followed a time course similar to that of estradiol (E2). Quantitative RT-PCR revealed that both BPA and E2 increased c-fos messenger RNA levels in the uterus 14- to 16-fold within 2 h, which returned to basal levels after 6 h. In the vagina, BPA-induced c-fos expression remained elevated for up to 6 h, compared with the transient increase caused by E2. Treatment of F344 rats for 3 days with continuous release capsules that supplied a much lower dose of BPA (approximately 0.3 mg/kg x day) resulted in hypertrophy, hyperplasia, and mucus secretion in the uterus and hyperplasia and cornification of the vaginal epithelium. The reproductive tract of SD rats did not respond to this treatment paradigm with BPA. These studies demonstrate that 1) the molecular and morphological alterations induced by BPA in the uterus and vagina are nearly identical to those induced by estradiol; 2) the vagina appears to be especially sensitive to the estrogenic actions of BPA; 3) the reproductive tract of the inbred F344 rat appears more sensitive to BPA than that of the outbred SD rat; and 4) continuous exposure to microgram levels of BPA is sufficient for exerting estrogenic actions.

摘要

已证实,异雌激素双酚A(BPA)在体内和体外均能模拟雌激素的作用。在雌激素敏感的Fischer 344大鼠(F344)中,BPA可刺激催乳素(PRL)分泌以及垂体后叶中一种PRL调节因子的表达,但在Sprague-Dawley(SD)大鼠中则无此作用。本研究的目的是检测BPA对生殖道的体内作用。具体目标为:1)描述BPA对子宫和阴道细胞增殖及c-fos表达的短期影响;2)比较长期低剂量暴露于BPA对F344和SD大鼠生殖道的影响。通过溴脱氧尿苷免疫染色确定,单次高剂量BPA处理可诱导去卵巢F344大鼠子宫和阴道细胞增殖。这种增殖呈剂量依赖性(37.5 - 150 mg/kg),且时间进程与雌二醇(E2)相似。定量逆转录聚合酶链反应(RT-PCR)显示,BPA和E2均可在2小时内使子宫中c-fos信使核糖核酸(mRNA)水平升高14至16倍,6小时后恢复至基础水平。在阴道中,与E2引起的短暂增加相比,BPA诱导的c-fos表达可持续升高长达6小时。用持续释放胶囊对F344大鼠进行3天处理,胶囊提供的BPA剂量低得多(约0.3 mg/kg·天),结果导致子宫肥大、增生和黏液分泌,以及阴道上皮增生和角化。SD大鼠的生殖道对这种BPA处理模式无反应。这些研究表明:1)BPA在子宫和阴道中诱导的分子和形态学改变与E2诱导的几乎相同;2)阴道似乎对BPA的雌激素作用特别敏感;3)近交系F344大鼠的生殖道对BPA似乎比远交系SD大鼠更敏感;4)持续暴露于微克水平的BPA足以发挥雌激素作用。

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