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测定和降低 17β-雌二醇、双酚 A 和壬基酚对斑马鱼卵黄蛋白原基因(vtg1)表达的雌激素潜力的预期寿命模型和分子对接分析。

Determination and reduced life expectancy model and molecular docking analyses of estrogenic potentials of 17β-estradiol, bisphenol A and nonylphenol on expression of vitellogenin gene (vtg1) in zebrafish.

机构信息

School of Environment, Jinan University, Guangzhou, 511443, China.

School of Environment, Jinan University, Guangzhou, 511443, China.

出版信息

Chemosphere. 2019 Apr;221:727-734. doi: 10.1016/j.chemosphere.2019.01.093. Epub 2019 Jan 16.

DOI:10.1016/j.chemosphere.2019.01.093
PMID:30677730
Abstract

This study determined and evaluated the estrogenic potentials on hepatic vitellogenin gene (vtg1) of adult male zebrafish which were exposed to low level concentrations (ng/L-μg/L levels) of individual and binary mixtures of 17β-estradiol (E), bisphenol A (BPA) and nonylphenol (NP) through the use of reduced life expectancy (RLE) model and molecular docking analysis. The order of in vivo estrogenic potentials of individual and binary exposure of E, BPA and NP was as follows: E+BPA>E>E+NP>BPA>BPA + NP >>>NP. Binary mixtures of E, BPA and NP had weak synergistic effects under the exposure concentration ranges. With the expression of hepatic vtg1 gene, the hepatic toxicity was analyzed by using the RLE model. All plots of the linear RLE model had negative slopes indicating that EC was negatively correlated with the natural logarithm of exposure time (lnET). The RLE model analyses can be useful to evaluate the exposure time effects of zebrafish by using EC as toxicity endpoint. Molecular docking analysis revealed that the interaction potential of E (Binding energy: -10.1 kcal/mol) for the zebrafish ERα-LBD was the most potent (stable), followed by BPA (-8.0 kcal/mol) and NP (-6.8 kcal/mol). Molecular docking analysis can be useful to understand interactive effects of E, BPA and NP.

摘要

本研究通过使用寿命缩短(RLE)模型和分子对接分析,确定并评估了暴露于低浓度(ng/L-μg/L 水平)的 17β-雌二醇(E)、双酚 A(BPA)和壬基酚(NP)的个体和二元混合物对成年雄性斑马鱼肝脏卵黄蛋白原基因(vtg1)的雌激素潜力。个体和二元暴露于 E、BPA 和 NP 的体内雌激素潜力顺序如下:E+BPA>E>E+NP>BPA>BPA+NP>NP。在暴露浓度范围内,E、BPA 和 NP 的二元混合物具有较弱的协同作用。通过 RLE 模型分析肝脏 vtg1 基因的表达,研究了肝脏毒性。线性 RLE 模型的所有图均具有负斜率,表明 EC 与暴露时间的自然对数(lnET)呈负相关。RLE 模型分析可用于通过将 EC 作为毒性终点来评估斑马鱼的暴露时间效应。分子对接分析表明,E(结合能:-10.1 kcal/mol)与斑马鱼 ERα-LBD 的相互作用潜力最强(稳定),其次是 BPA(-8.0 kcal/mol)和 NP(-6.8 kcal/mol)。分子对接分析可用于了解 E、BPA 和 NP 的相互作用效应。

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