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人肝微粒体对四种有机磷硫代酸酯类农药的细胞色素P450特异性生物活化作用。

CYP-specific bioactivation of four organophosphorothioate pesticides by human liver microsomes.

作者信息

Buratti Franca M, Volpe Maria Teresa, Meneguz Annarita, Vittozzi Luciano, Testai Emanuela

机构信息

Comparative Toxicology and Ecotoxicology Laboratory, Istituto Superiore di Sanità, Viale Regina Elena 299, I-00161 Rome, Italy.

出版信息

Toxicol Appl Pharmacol. 2003 Feb 1;186(3):143-54. doi: 10.1016/s0041-008x(02)00027-3.

Abstract

The bioactivation of azinphos-methyl (AZIN), chlorpyrifos (CPF), diazinon (DIA), and parathion (PAR), four widely used organophosphorothioate (OPT) pesticides has been investigated in human liver microsomes (HLM). In addition, the role of human cytochrome P450 (CYPs) in OPT desulfuration at pesticide levels representative of human exposure have been defined by means of correlation and immunoinhibition studies. CYP-mediated oxon formation from the four OPTs is efficiently catalyzed by HLM, although showing a high variability (>40-fold) among samples. Two distinct phases were involved in the desulfuration of AZIN, DIA, and PAR, characterized by different affinity constants (K(mapp1) = 0.13-9 microM and K(mapp2) = 5- 269 microM). Within the range of CPF concentrations tested, only the high-affinity component was evidenced (K(mapp1) = 0.27-0.94 microM). Oxon formation in phenotyped individual HLM showed a significant correlation with CYP1A2-, 3A4-, and 2B6-related activities, at different levels depending on the OPT concentration. Anti-human CYP1A2, 2B6, and 3A4 antibodies significantly inhibited oxon formation, showing the same OPT concentration dependence. Our data indicated that CYP1A2 is mainly involved in OPT desulfuration at low pesticide concentrations, while the role of CYP3A4 is more significant to the low-affinity component of OPT bioactivation. The contribution of CYP2B6 to total hepatic oxon formation was relevant in a wide range of pesticide concentrations, being a very efficient catalyst of both the high- and low-affinity phase. These results suggest CYP1A2 and 2B6 as possible metabolic biomarkers of susceptibility to OPT toxic effect at the actual human exposure levels.

摘要

已在人肝微粒体(HLM)中研究了谷硫磷(AZIN)、毒死蜱(CPF)、二嗪农(DIA)和对硫磷(PAR)这四种广泛使用的有机磷硫代酯(OPT)农药的生物活化作用。此外,通过相关性和免疫抑制研究确定了人细胞色素P450(CYPs)在代表人体暴露的农药水平下对OPT脱硫作用中的作用。尽管样品间显示出高变异性(>40倍),但HLM能有效催化CYP介导的这四种OPT形成氧磷。AZIN、DIA和PAR的脱硫涉及两个不同阶段,其特征在于不同的亲和常数(K(mapp1)=0.13 - 9 microM和K(mapp2)=5 - 269 microM)。在所测试的CPF浓度范围内,仅证明了高亲和力成分(K(mapp1)=0.27 - 0.94 microM)。在表型化的个体HLM中氧磷形成与CYP1A2、3A4和2B6相关活性呈显著相关,具体水平取决于OPT浓度。抗人CYP1A2、2B6和3A4抗体显著抑制氧磷形成,呈现相同的OPT浓度依赖性。我们的数据表明,CYP1A2主要在低农药浓度下参与OPT脱硫,而CYP3A4对OPT生物活化的低亲和力成分作用更显著。CYP2B6对肝脏总氧磷形成的贡献在广泛的农药浓度范围内都很显著,是高亲和力和低亲和力阶段的高效催化剂。这些结果表明,在实际人体暴露水平下,CYP1A2和2B6可能是对OPT毒性作用易感性的潜在代谢生物标志物。

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