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CYP450 Enzyme-Mediated Metabolism of TCAS and Its Inhibitory and Induced Effects on Metabolized Enzymes inVitro

机译:CYP450酶介导的TCAS代谢及其对代谢酶的抑制和诱导作用体外

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摘要

In this study, we investigated the enzymes catalyzing the phaseⅠmetabolism of thiacalixarene (TCAS) based on in vitro system including cDNA-expressed P450 enzymes, human liver microsomes plus inhibitors and monoclonal antibodies. In addition, the inhibitory potential of TCAS on major CYP450 drug metabolizing enzymes (CYP1A2, CYP2C9, CYP2B6, CYP2D6 and CYP3A4) was assessed. The results showed that CYP1A2 and CYP2C9 mediated TCAS hydroxylation. IC50 values for TCAS in rat and human liver microsomes were greater than 50 µM, and it demonstrated a weak inhibition of rat and human CYP450 enzymes. Finally, sandwiched hepatocytes were used to evaluate the induction of CYP1A and CYP3A to define the function of TCAS in vivo. The results showed that incubation of TCAS at different concentrations for 72 h failed to induce CYP1A and CYP3A. However, incubation of the cells with 50 and 100 µM TCAS caused a profound decrease in the activities of CYP1A and CYP3A, which was probably due to cytotoxic effects, suggesting that exposure to TCAS might be a health concern.
机译:本研究基于体外系统研究了催化噻唑烷芳烃(TCAS)Ⅰ相代谢的酶,包括表达cDNA的P450酶,人肝微粒体及抑制剂和单克隆抗体。此外,评估了TCAS对主要CYP450药物代谢酶(CYP1A2,CYP2C9,CYP2B6,CYP2D6和CYP3A4)的抑制潜力。结果表明CYP1A2和CYP2C9介导TCAS羟基化。大鼠和人肝微粒体中TCAS的IC50值大于50 µM,表明对大鼠和人CYP450酶的抑制作用较弱。最后,将夹心的肝细胞用于评估CYP1A和CYP3A的诱导作用,以定义TCAS在体内的功能。结果表明,不同浓度的TCAS孵育72小时均未诱导CYP1A和CYP3A。然而,将细胞与50和100 µM TCAS一起孵育会导致CYP1A和CYP3A的活性大大降低,这可能是由于细胞毒性作用所致,这表明暴露于TCAS可能是健康问题。

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