首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Impact of oral bisphenol A at reference doses on intestinal barrier function and sex differences after perinatal exposure in rats
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Impact of oral bisphenol A at reference doses on intestinal barrier function and sex differences after perinatal exposure in rats

机译:参考剂量口服双酚A对围产期大鼠暴露后肠道屏障功能和性别差异的影响

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摘要

Bisphenol A (BPA), a chemical estrogen widely used in the food-packaging industry and baby bottles, is recovered in human fluids (0.1–10 nM). Recent studies have reported that BPA is hormonally active at low doses, emphasizing the debate of a risk for human health. Estrogen receptors are expressed in the colon, and although the major route of BPA exposure is food, the effects on gut have received no attention. We first examined the endocrine disrupting potency of BPA on colonic paracellular permeability (CPP), experimental colitis, and visceral sensitivity in ovariectomized rats orally exposed to 5 mg/kg/d BPA (i.e., the no observed adverse effect level), 50 μg/kg/d BPA (i.e., tolerable daily intake), or lower doses. BPA dose-dependently decreased basal CPP, with a half-maximal inhibitory dose of 5.2 μg/kg/d, 10-fold below the tolerable daily intake. This correlated with an increase in epithelial tight junction sealing, also observed in Caco-2 cells exposed to 10 nM BPA. When ovariectomized rats were fed with BPA at the no observed adverse effect level, the severity of colitis was reduced, whereas the same dose increased pain sensitivity to colorectal stimuli. We then examined the impact of perinatal exposure to BPA on intestinal permeability and inflammatory response in the offspring. In female rats, but not in male rats, perinatal BPA evoked a decrease of CPP in adulthood, whereas the proinflammatory response of colonic mucosa was strengthened. This study first demonstrates that the xenoestrogen BPA at reference doses influences intestinal barrier function and gut nociception. Moreover, perinatal exposure promotes the development of severe inflammation in adult female offspring only.
机译:双酚A(BPA)是一种化学雌激素,广泛用于食品包装行业和婴儿奶瓶中,可从人的体液中回收(0.1-10 nM)。最近的研究报告说,低剂量的双酚A具有激素活性,强调了对人类健康风险的争论。雌激素受体在结肠中表达,尽管BPA暴露的主要途径是食物,但对肠道的影响尚未引起关注。我们首先检查了口服暴露于5 mg / kg / d BPA(未观察到的不良反应水平),50μg/ kg的去卵巢大鼠的BPA对结肠副细胞通透性(CPP),实验性结肠炎和内脏敏感性的内分泌破坏能力。 kg / d BPA(即每日容许摄入量)或更低剂量。 BPA剂量依赖性降低基础CPP,最大抑制剂量为5.2μg/ kg / d,是可耐受的每日摄入量的10倍。这与上皮紧密连接密封的增加相关,这在暴露于10 nM BPA的Caco-2细胞中也观察到。当在未观察到不良反应水平的情况下给切除卵巢的大鼠喂食BPA时,结肠炎的严重程度降低了,而相同剂量增加了对结直肠刺激的疼痛敏感性。然后,我们检查了围产期接触BPA对后代肠道通透性和炎症反应的影响。在雌性大鼠中,而非雌性大鼠中,围产期BPA引起成年CPP降低,而结肠粘膜的促炎反应增强。这项研究首先证明了参考剂量的异雌激素BPA影响肠屏障功能和肠道伤害感受。此外,围产期暴露仅促进成年雌性后代严重炎症的发展。

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