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有机磷杀虫剂与人血清白蛋白相互作用的机制:固相微萃取、热力学和计算方法。

Mechanism of interactions between organophosphorus insecticides and human serum albumin: Solid-phase microextraction, thermodynamics and computational approach.

机构信息

Institute of Quality and Standards for Agricultural Products, Zhejiang Academy of Agricultural Sciences, Hangzhou, China.

Department of Pharmacodynamics and Molecular Pharmacology, Nicolaus Copernicus University, Toruń, Poland.

出版信息

Chemosphere. 2020 Aug;253:126698. doi: 10.1016/j.chemosphere.2020.126698. Epub 2020 Apr 7.

Abstract

Organophosphates insecticides (OPs) are one of the major environmental pollutants and their interaction with human serum albumin (HSA) has been shown to have significant effects on their bioavailability which is related to toxicokinetics and toxicodynamics in human body. In this research, solid-phase microextraction methods were developed to analyse the free concentrations of three OPs (chlorpyrifos, parathion-methyl and malathion) in buffered HSA solution and that provide a useful method for the determination of binding affinity constants (K), binding forces and binding location. Polydimethylsiloxane fibers were selected for analysing the free concentrations of OPs, with an external calibration approach. Good linearities conducted in PBS solution were observed in the range of 0.0025-1.7 μmol L (R = 0.9975) for chlorpyrifos, 1.0-27 μmol L (R = 0.9974) for parathion-methyl, and 0.5-70 μmol L (R = 0.9973)for malathion, respectively. The LODs for instrument response were 1 ng, 5 ng and 10 ng for chlorpyrifos, parathion-methyl and malathion, respectively. The K values for chlorpyrifos, parathion-methyl and malathion showed that they were positively correlated with hydrophobicity and negatively correlated with temperature. The OP binding sites on HSA were confirmed by site marker competition test and further proven by computational approaches. The recognition region of parathion-methyl was situated within residues 199-292 in subdomain IIA. Malathion bonded to residues 404-558 in subdomain IIIA. The mode of action between HSA-parathion-methyl and HSA-malathion is found to involve mainly by H-bonds, π-π stacking and hydrophobic effects. These results clearly demonstrate the noncovalent binding of OPs with HSA and provide new insight into solid-phase microextraction, thermodynamics and computational approaches.

摘要

有机磷杀虫剂(OPs)是主要的环境污染物之一,它们与人体血清白蛋白(HSA)的相互作用已被证明对其生物利用度有显著影响,而生物利用度与人体的毒代动力学和毒效动力学有关。在这项研究中,开发了固相微萃取方法来分析缓冲 HSA 溶液中三种 OPs(毒死蜱、甲基对硫磷和马拉硫磷)的游离浓度,为测定结合亲和力常数(K)、结合力和结合位置提供了一种有用的方法。选择聚二甲基硅氧烷纤维分析 OPs 的游离浓度,采用外部校准方法。在 PBS 溶液中观察到良好的线性关系,范围为 0.0025-1.7 μmol·L(R=0.9975)的毒死蜱、1.0-27 μmol·L(R=0.9974)的甲基对硫磷和 0.5-70 μmol·L(R=0.9973)的马拉硫磷。仪器响应的 LOD 分别为 1ng、5ng 和 10ng 的毒死蜱、甲基对硫磷和马拉硫磷。氯吡硫磷、甲基对硫磷和马拉硫磷的 K 值表明,它们与疏水性呈正相关,与温度呈负相关。通过位点标记竞争试验和计算方法进一步证实了 HSA 上 OPs 的结合位点。甲基对硫磷的识别区域位于 IIA 亚结构域的 199-292 残基内。马拉硫磷与 IIIA 亚结构域的 404-558 残基结合。发现 HSA-甲基对硫磷和 HSA-马拉硫磷之间的作用模式主要涉及氢键、π-π堆积和疏水相互作用。这些结果清楚地表明 OPs 与 HSA 的非共价结合,并为固相微萃取、热力学和计算方法提供了新的见解。

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