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Dioxybenzone triggers enhanced estrogenic effect via metabolic activation: in silico, in vitro and in vivo investigation

机译:二氧苯脲触发通过代谢活化增强雌激素效果:在硅,体外和体内调查中

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摘要

Dioxybenzone is widely used in cosmetics and personal care products and frequently detected in multiple environmental media and human samples. However, the current understanding of the metabolic susceptibility of dioxybenzone and the potential endocrine disruption through its metabolites in mimicking human estrogens remains largely unclear. Here we investigated the in vitro metabolism of dioxybenzone, detected the residue of metabolites in rats, and determined the estrogenic disrupting effects of these metabolites toward estrogen receptor alpha (ER alpha). In vitro metabolism revealed two major metabolites from dioxybenzone, i.e., M1 through the demethylation of methoxy moiety and M2 through hydroxylation of aromatic carbon. M1 and M2 were both rapidly detected in rat plasma upon exposure to dioxybenzone, which were then distributed into organs of rats in the order of livers kidneys uteri ovaries. The 100 ns molecular dynamics simulation revealed that M1 and M2 formed hydrogen bond to residue Leu387 and Glu353, respectively, on ERa ligand binding domain, leading to a reduced binding free energy. M1 and M2 also significantly induced estrogenic effect in comparison to dioxybenzone as validated by the recombinant ERa yeast two-hybrid assay and uterotrophic assay. Overall, our study revealed the potential of metabolic activation of dioxybenzone to induce estrogenic disrupting effects, suggesting the need for incorporating metabolic evaluation into the health risk assessment of benzophenones and their structurally similar analogs. (C) 2020 Elsevier Ltd. All rights reserved.
机译:二恶英脲广泛应用于化妆品和个人护理产品,并经常在多种环境媒体和人类样品中检测到。然而,目前通过其代谢物模仿人雌性的代谢产物对二恶英苯脲的代谢易感性以及潜在的内分泌破坏的理解仍然很目前不清楚。在这里,我们研究了二恶英苯的体外代谢,检测到大鼠代谢物的残留物,并确定这些代谢物对雌激素受体α(ERα)的雌激素破坏效应。体外代谢揭示了二氧氧脲的两种主要代谢产物,即通过甲氧基部分的去甲基化通过芳族碳的羟基化的甲氧基部分和M2的脱甲基化。在暴露于二恶英中,在大鼠等离子体上迅速检测到M1和M2,然后在肝脏>肾脏的序列中分布到大鼠的器官中,然后肾脏>卵巢>卵巢。 100ns分子动力学模拟显示M1和M2分别在ERA配体结合结构域上分别对残基Leu387和Glu353形成的氢键,导致减少的无结合能量。与通过重组时代酵母双杂交测定和子宫营养测定验证的二恶氧脲相比,M1和M2也显着诱导了雌激素效果。总体而言,我们的研究揭示了二氧氧脲代谢活化以诱导雌激素破坏效应的潜力,表明需要将代谢评估纳入二苯甲酸酮及其结构类似类似物的健康风险评估。 (c)2020 elestvier有限公司保留所有权利。

著录项

  • 来源
    《Environmental Pollution》 |2021年第2期|115766.1-115766.9|共9页
  • 作者单位

    Zhejiang Univ Coll Environm & Resource Sci Key Lab Environm Remediat & Ecol Hlth Minist Educ Hangzhou 310058 Peoples R China;

    IBM Thomas J Watson Res Ctr Computat Biol Ctr Yorktown Hts NY USA;

    Zhejiang Univ Coll Environm & Resource Sci Key Lab Environm Remediat & Ecol Hlth Minist Educ Hangzhou 310058 Peoples R China;

    Zhejiang Univ Coll Environm & Resource Sci Key Lab Environm Remediat & Ecol Hlth Minist Educ Hangzhou 310058 Peoples R China;

    Zhejiang Univ Inst Quantitat Biol Hangzhou 310058 Peoples R China|Zhejiang Univ Coll Life Sci Hangzhou 310058 Peoples R China|Columbia Univ Dept Chem New York NY 10027 USA;

    Zhejiang Univ Coll Environm & Resource Sci Key Lab Environm Remediat & Ecol Hlth Minist Educ Hangzhou 310058 Peoples R China;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    Dioxybenzone; Metabolism; Estrogenic effect; Molecular modeling; Mass spectrometry;

    机译:二氧苯脲;新陈代谢;雌激素效果;分子建模;质谱;

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