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低剂量双酚 AF 通过复杂机制对哺乳动物睾丸发育产生影响:在婴儿期和成年期都可检测到这些变化。

Effects of low-dose bisphenol AF on mammal testis development via complex mechanisms: alterations are detectable in both infancy and adulthood.

机构信息

State Key Laboratory of Environmental Chemistry and Ecotoxicology, Research Center for Eco-environmental Sciences, Chinese Academy of Sciences, No. 18, Shuangqing Road, Haidian, 100085, Beijing, China.

University of Chinese Academy of Sciences, Beijing, 100049, China.

出版信息

Arch Toxicol. 2022 Dec;96(12):3373-3383. doi: 10.1007/s00204-022-03377-0. Epub 2022 Sep 13.

Abstract

Despite growing concern about adverse effects of bisphenol AF (BPAF) due to its endocrine disrupting properties, there is a lack of toxicity data from low-dose studies and direct evidence linking its adverse effects to endocrine disrupting properties. Here, we investigated the effects of gestational and postnatal exposure to BPAF through drinking water (0.15-15 μg/mL, equivalent to the daily intake of ~ 50 and 5 mg/kg/day) on testis development in mice. We found that like mestranol, 5 mg/kg/day BPAF resulted in remarkable decreases in multiple male reproductive parameters in adulthood, such as the sperm number and serum testosterone level. Notably, 50 μg/kg/day BPAF also caused significant decreases in anogenital distance (AGD), the luteinizing hormone level and spermatocyte number, along with declining trends in sperm number and the serum levels of testosterone and follicle-stimulating hormone. In line with the adverse outcomes observed in adulthood, on postnatal day (PND) 9, we also observed BPAF-caused dose-dependent alterations, including reduced AGD, seminiferous tubule area and numbers of total germ cells, spermatocytes and Leydig cells, coupled with down-regulated expression of male-biased genes in testes. Even when exposure to 5 mg/kg/day BPAF as well as MES was initiated from PND 0, similar alterations in male reproductive parameters were also found on PND 9, along with a decrease in the GnRH content in the hypothalamus; moreover, testicular alterations and the reduction in AGD were partly antagonized by the estrogen receptor (ER) antagonist ICI 182,780, but the reduction of GnRH production was not done, showing that the effects of BPAF on testis development may be partially mediated by ER signaling. In conclusion, all the findings demonstrate that low-dose BPAF can partly disrupt mammal testis development and cause adverse testicular outcomes in adulthood, indicating a potential reproductive risk to mammals including humans. Importantly, our finding that developmental alterations elicited by BPAF have been detectable on PND 9 provides important motivation for the development of effective methods for early detection of adverse effects of estrogenic chemicals on testis development.

摘要

尽管双酚 AF(BPAF)因其内分泌干扰特性而引起人们对其不良影响的日益关注,但缺乏低剂量研究的毒性数据,也没有直接证据将其不良影响与其内分泌干扰特性联系起来。在这里,我们通过饮用水(0.15-15μg/ml,相当于每天摄入约 50 和 5mg/kg/天)研究了妊娠期和产后暴露于 BPAF 对小鼠睾丸发育的影响。我们发现,与美雌醇一样,5mg/kg/天的 BPAF 导致成年雄性生殖参数显著下降,例如精子数量和血清睾酮水平。值得注意的是,50μg/kg/天的 BPAF 还导致肛殖距离(AGD)、促黄体生成素水平和精母细胞数量显著下降,同时精子数量和血清睾酮和卵泡刺激素水平呈下降趋势。与成年期观察到的不良结果一致,在产后第 9 天(PND),我们还观察到 BPAF 引起的剂量依赖性改变,包括 AGD 降低、曲细精管面积和总生殖细胞、精母细胞和间质细胞数量减少,以及睾丸中雄性偏倚基因表达下调。即使从 PND0 开始暴露于 5mg/kg/天的 BPAF 和 MES,在 PND9 时也发现雄性生殖参数的类似改变,同时下丘脑 GnRH 含量下降;此外,睾丸改变和 AGD 降低部分被雌激素受体(ER)拮抗剂 ICI 182,780 拮抗,但 GnRH 产生的减少未被拮抗,表明 BPAF 对睾丸发育的影响可能部分通过 ER 信号传递。总之,所有研究结果表明,低剂量的 BPAF 可部分干扰哺乳动物睾丸发育,并导致成年后睾丸不良结局,表明 BPAF 对包括人类在内的哺乳动物具有潜在的生殖风险。重要的是,我们发现 BPAF 引起的发育改变在 PND9 时已经可以检测到,这为开发有效方法早期检测雌激素类化学物质对睾丸发育的不良影响提供了重要动力。

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