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高效液相色谱-四极杆飞行时间质谱代谢组学研究马拉硫磷对映体、外消旋体和代谢物对 HepG2 细胞的不同毒性作用。

Different Toxic Effects of Racemate, Enantiomers, and Metabolite of Malathion on HepG2 Cells Using High-Performance Liquid Chromatography-Quadrupole-Time-of-Flight-Based Metabolomics.

出版信息

J Agric Food Chem. 2019 Feb 20;67(7):1784-1794. doi: 10.1021/acs.jafc.8b04536. Epub 2019 Feb 8.

Abstract

Commercial malathion is a racemic mixture that contains two enantiomers, and malathion has adverse effects on mammals. However, whether these two enantiomers have different effects on animals remains unclear. In this study, we tested the effect of racemate, enantiomers, and metabolite of malathion on the metabolomics profile of HepG2 cells. HepG2 cells showed distinct metabolic profiles when treated with rac-malathion, malaoxon, R-(+)-malathion, and S-(-)-malathion, and these differences were attributed to pathways in amino acid metabolism, oxidative stress, and inflammatory response. In addition, malathion treatment caused changes in amino acid levels, antioxidant activity, and expression of inflammatory genes in HepG2 cells. S-(-)-Malathion exhibited stronger metabolic perturbation than its enantiomer and racemate, consistent with the high level of cytotoxicity of S-(-)malathion. R-(+)-Malathion treatment caused significant oxidative stress in HepG2 cells but induced a weaker disturbance in the amino acid metabolism and a pro-inflammatory response compared to S-(-)-malathion and rac-malathion. Malaoxon caused more significant perturbation on antioxidase and a stronger antiapoptosis effect than its parent malathion. Our results provide insight into the risk assessment of malathion enantiomers and metabolites. We also demonstrate that a metabolomics approach can identify the discrepancy of the toxic effects and underlying mechanisms for enantiomers and metabolites of chiral pesticides.

摘要

商业用马拉硫磷是一种外消旋混合物,其中包含两种对映异构体,马拉硫磷对哺乳动物有不良影响。然而,这两种对映异构体对动物是否有不同的影响尚不清楚。在这项研究中,我们测试了马拉硫磷的外消旋体、对映异构体和代谢物对 HepG2 细胞代谢组学图谱的影响。当用 rac-马拉硫磷、马拉氧磷、R-(+)-马拉硫磷和 S-(-)-马拉硫磷处理 HepG2 细胞时,细胞表现出明显不同的代谢谱,这些差异归因于氨基酸代谢、氧化应激和炎症反应途径。此外,马拉硫磷处理导致 HepG2 细胞中氨基酸水平、抗氧化活性和炎症基因表达的变化。S-(-)-马拉硫磷比其对映异构体和外消旋体表现出更强的代谢扰动,这与 S-(-)马拉硫磷的高细胞毒性水平一致。与 S-(-)-马拉硫磷和 rac-马拉硫磷相比,R-(+)-马拉硫磷处理在 HepG2 细胞中引起显著的氧化应激,但在氨基酸代谢和促炎反应方面引起的干扰较弱。马拉氧磷比其母体马拉硫磷引起更显著的抗氧化酶扰动和更强的抗凋亡作用。我们的结果为马拉硫磷对映异构体和代谢物的风险评估提供了深入的了解。我们还表明,代谢组学方法可以识别手性农药对映异构体和代谢物的毒性作用和潜在机制的差异。

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