首页> 美国卫生研究院文献>Environmental Health Perspectives >Relative binding affinity-serum modified access (RBA-SMA) assay predicts the relative in vivo bioactivity of the xenoestrogens bisphenol A and octylphenol.
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Relative binding affinity-serum modified access (RBA-SMA) assay predicts the relative in vivo bioactivity of the xenoestrogens bisphenol A and octylphenol.

机译:相对结合亲和力-血清修饰通路(RBA-SMA)测定法可预测异种雌激素双酚A和辛基酚的相对体内生物活性。

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摘要

We have developed a relative binding affinity-serum modified access (RBA-SMA) assay to determine the effect of serum on the access of xenoestrogens to estrogen receptors within intact cultured MCF-7 human breast cancer cells. We used this assay to predict low dose activity of two xenoestrogens in mice. In serum-free medium, bisphenol A, a component of polycarbonates and of resins used to line metal food cans, showed a lower relative binding affinity (RBA; 0.006%) than octylphenol (0.072%) and nonylphenol (0.026%), which are used as surfactants in many commercial products (all RBAs are relative to estradiol, which is equal to 100%). In 100% serum from adult men, bisphenol A showed a higher RBA (0.01%) than in serum-free medium and thus enhanced access to estrogen receptors relative to estradiol. In contrast, octylphenol showed a 22-fold decrease in RBA (0.0029%) and nonylphenol showed a 5-fold decrease in RBA (0.0039%) when measured in adult serum. This indicates that, relative to estradiol, serum had less of an inhibitory effect on the cell uptake and binding in MCF-7 cells of bisphenol A, while serum had a greater inhibitory effect on octylphenol and nonylphenol relative to estradiol. Extrapolation of these relative activities in adult serum predicted that the estrogenic bioactivity of bisphenol A would be over 500-fold greater than that of octylphenol in fetal mouse serum. Bisphenol A and octylphenol were fed to pregnant mice at 2 and 20 micrograms/kg/day. Exposure of male mouse fetuses to either dose of bisphenol A, but to neither dose of octylphenol, significantly increased their adult prostate weight relative to control males, which is consistent with the higher predicted bioactivity of bisphenol A than octylphenol in the RBA-SMA assay. In addition, our findings show for the first time that fetal exposure to environmentally relevant parts-per-billion (ppb) doses of bisphenol A, in the range currently being consumed by people, can alter the adult reproductive system in mice.
机译:我们已经开发了相对结合亲和力-血清修饰通路(RBA-SMA)测定法,以测定血清对异种雌激素对完整培养的MCF-7人乳腺癌细胞内雌激素受体的通路的影响。我们使用该测定法预测了小鼠中两种异雌激素的低剂量活性。在无血清培养基中,双酚A(一种聚碳酸酯和用于金属食品罐衬里的树脂的一种成分)相对于辛基酚(0.072%)和壬基酚(0.026%)具有较低的相对结合亲和力(RBA; 0.006%)。在许多商业产品中用作表面活性剂(所有RBA都相对于雌二醇,等于100%)。在成年男性的100%血清中,双酚A的RBA(0.01%)比无血清的培养基高,因此相对于雌二醇,双酚A的雌激素受体获得率更高。相反,在成人血清中进行测定时,辛基苯酚的RBA降低了22倍(0.0029%),壬基苯酚的RBA降低了5倍(0.0039%)。这表明,相对于雌二醇,血清对双酚A的MCF-7细胞的细胞摄取和结合的抑制作用较小,而血清对雌二醇的辛基苯酚和壬基酚的抑制作用较大。对成人血清中这些相对活性的推断表明,双酚A的雌激素生物活性将比胎儿小鼠血清中的辛基酚高500倍以上。将双酚A和辛基苯酚以2和20微克/ kg /天的剂量喂给怀孕的小鼠。相对于对照雄性,将雄性小鼠胎儿暴露于任一剂量的双酚A但不暴露于辛基酚的情况下,它们的成年前列腺重量显着增加,这与RBA-SMA分析中双酚A的预测生物活性高于辛基酚的预测生物活性相符。此外,我们的研究结果首次表明,胎儿暴露于与环境相关的十亿分之一(ppb)剂量的双酚A(在人们目前所消耗的范围内)可以改变小鼠的成年生殖系统。

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