细胞色素CYP1A和CYP3A在苯并(a)芘遗传毒性作用中的作用

D. A. Malygina, Nadezhda Yurievna Rogovskaya, P. Beltyukov, V. Babakov
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摘要

介绍。苯并(a)芘代谢物是遗传毒性化合物,其积累有助于致癌。代谢产物形成的主要机制是细胞色素P450 (CYP)氧化苯并(a)芘。主要细胞色素的抑制剂可以降低代谢物形成的速率,从而降低苯并(a)芘代谢物的遗传毒性作用。相反,细胞色素诱导剂有助于增强遗传毒性。目标。这项工作的目的是建立一个基于HepaRG细胞的细胞模型,以研究细胞色素活性在苯并(a)芘遗传毒性作用中的作用。材料和方法。为了评估细胞色素CYP3A和CYP1A抑制剂对苯并(a)芘在HepaRG细胞中的遗传毒性作用的影响,利用Luminex xMAP技术通过免疫分析法测定了DNA损伤检测和修复系统活性蛋白的含量,磷酸化形式的信号级联蛋白。采用xCelligence分析仪实时细胞分析评价苯并(a)芘的细胞毒性。结果。CYP3A和CYP1A细胞色素抑制剂、酮康唑和α-萘黄酮能够减弱苯(a)芘的毒性作用,降低DNA修复系统的激活,并对信号通路中不同酪氨酸激酶的磷酸化具有多向作用。结论。HepaRG人肝癌细胞是一个合适的细胞模型,既可以评估细胞色素对异种生物代谢的贡献,也可以研究细胞色素抑制剂对苯并(a)芘基因毒性作用的细胞保护作用。的局限性。这项研究是在细胞培养上进行的。为了将数据外推到生物体,有必要考虑到毒物动力学和毒物动力学的数据。
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The role of cytochromes CYP1A and CYP3A in the genotoxic effect of benzo(a)pyrene
Introduction. Benzo(a)pyrene metabolites are genotoxic compounds, the accumulation of which contributes to carcinogenesis. The main mechanism of metabolite formation is the benzo(a)pyrene oxidation by cytochromes P450 (CYP). Inhibitors of the main cytochromes can reduce the rate of metabolite formation and, as a result, to decrease the genotoxic effects of benzo(a)pyrene metabolites. In contrast, inducers of cytochromes contribute to the enhancement of genotoxicity. Objective. The aim of the work was to develop a cell model based on the HepaRG cells to study the role of cytochromes activity in the genotoxic effect of benzo (a) pyrene. Material and methods. To assess the effect of inhibitors of cytochromes CYP3A and CYP1A on the genotoxic effect of benzo(a)pyrene in HepaRG cells, the content of active forms of proteins of the DNA damage detection and repair system, phosphorylated forms of signaling cascade proteins was determined by immunoassay using Luminex xMAP technology. The cytotoxicity of benzo(a)pyrene was assessed by real-time cell analysis on xCelligence analyzer. Results. Inhibitors of CYP3A and CYP1A cytochromes, ketoconazole and α-naphthoflavone demonstrate the ability to diminish the toxic effects of benz (a) pyrene, reduce the activation of the DNA repair system, and have a multidirectional effect on the different tyrosine kinases phosphorylation in signaling pathways. Conclusion. HepaRG human hepatoma cells are a suitable cell model both to assess the contribution of cytochromes to the metabolism of xenobiotics and to study of the cell protection from the genotoxic effect of benzo (a) pyrene by cytochrome inhibitors. Limitations. The study was performed on a cell culture. To extrapolate the data to the organism, it is necessary to take into account the data of toxicodynamics and toxicokinetics.
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