Department of Chemistry and Toxicology, Veterinary Research Institute, Hudcova 70, 62100 Brno, Czech Republic.
Chem Res Toxicol. 2011 Jun 20;24(6):866-76. doi: 10.1021/tx200049x. Epub 2011 Jun 3.
The methylated benzo[a]pyrenes (MeBaPs) are present at significant levels in the environment, especially in the sediments contaminated by petrogenic PAHs. However, the existing data on their toxic effects in vitro and/or in vivo are still largely incomplete. Transcription factor AhR plays a key role in the metabolic activation of PAHs to genotoxic metabolites, but the AhR activation may also contribute to the tumor promoting effects of PAHs. In this study, the AhR-mediated activity of five selected MeBaP isomers was estimated in the DR-CALUX reporter gene assay performed in rat hepatoma cells. Detection of other effects, including induction of CYP1A1, CYP1B1, and AKR1C9 mRNAs, DNA adduct formation, production of reactive oxygen species, oxidation of deoxyguanosine, and cell cycle modulation and apoptosis, was performed in the rat liver epithelial WB-F344 cell line, a model of liver progenitor cells. We identified 1-MeBaP as the most potent inducer of AhR activation, stable DNA adduct formation, checkpoint kinase 1 and p53 phosphorylation, and apoptosis. These effects suggest that 1-MeBaP is a potent genotoxin eliciting a typical sequence of events ascribed to carcinogenic PAHs: induction of CYP1 enzymes, formation of high levels of DNA adducts, activation of DNA damage responses (including p53 phosphorylation), and cell death. In contrast, 10-MeBaP, representing BaP isomers substituted with the methyl group in the angular ring, elicited only low levels DNA adduct formation and apoptosis. Other MeBaPs under study also elicited strong apoptotic responses associated with DNA adduct formation as the prevalent mode of toxic action of these compounds in liver cells. MeBaPs induced a weak production of ROS, which did not lead to significant oxidative DNA damage. Importantly, 1-MeBaP and 3-MeBaP were found to be potent AhR agonists, one order of magnitude more potent than BaP, thus suggesting that the AhR-dependent modulations of gene expression, deregulation of cell survival mechanisms, and further nongenotoxic effects associated with AhR activation may further contribute to their tumor promotion and carcinogenicity.
甲基苯并[a]蒽(MeBaPs)在环境中含量很高,特别是在受石油源多环芳烃污染的沉积物中。然而,目前关于其在体外和/或体内的毒性效应的数据仍然很不完整。转录因子 AhR 在多环芳烃代谢激活为遗传毒性代谢物中起着关键作用,但 AhR 的激活也可能导致多环芳烃的肿瘤促进作用。在这项研究中,在大鼠肝癌细胞中进行的 DR-CALUX 报告基因检测中,评估了五种选定的 MeBaP 异构体的 AhR 介导活性。在大鼠肝上皮 WB-F344 细胞系中,还检测了其他效应,包括 CYP1A1、CYP1B1 和 AKR1C9 mRNA 的诱导、DNA 加合物形成、活性氧的产生、脱氧鸟苷的氧化以及细胞周期调节和细胞凋亡。WB-F344 细胞系是肝祖细胞的模型。我们发现 1-MeBaP 是 AhR 激活、稳定的 DNA 加合物形成、检查点激酶 1 和 p53 磷酸化以及细胞凋亡的最有效诱导剂。这些效应表明,1-MeBaP 是一种有效的遗传毒物,引发了归因于致癌多环芳烃的典型事件序列:CYP1 酶的诱导、高水平 DNA 加合物的形成、DNA 损伤反应的激活(包括 p53 磷酸化)和细胞死亡。相比之下,代表在角环中用甲基取代的 BaP 异构体的 10-MeBaP 仅引起低水平的 DNA 加合物形成和细胞凋亡。在所研究的其他 MeBaPs 也引起强烈的凋亡反应,与这些化合物在肝细胞中的主要毒性作用方式是 DNA 加合物形成有关。MeBaPs 诱导产生较弱的 ROS,这不会导致明显的氧化 DNA 损伤。重要的是,1-MeBaP 和 3-MeBaP 被发现是有效的 AhR 激动剂,比 BaP 强一个数量级,这表明 AhR 依赖性基因表达的调节、细胞存活机制的失调以及与 AhR 激活相关的进一步非遗传毒性效应可能进一步有助于它们的肿瘤促进和致癌性。
