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The Alternaria mycotoxins alternariol and alternariol methyl ether induce cytochrome P450 1A1 and apoptosis in murine hepatoma cells dependent on the aryl hydrocarbon receptor

机译:链格孢霉毒素和链格孢杆菌甲醚可诱导小鼠肝癌细胞中的细胞色素P450 1A1和细胞凋亡,取决于芳烃受体

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The Alternaria mycotoxins alternariol (AOH) and alternariol methyl ether (AME) are potential carcinogens. As planar compounds, AOH and AME are preferentially metabolized by cytochrome P450 (CYP) 1A1 and 1A2. The most prominent regulator of CYP1A1 is the dimeric transcription factor complex AhR/ARNT, which is activated by planar ligands. Therefore, we studied the activation of AhR/ARNT by AOH and AME and monitored CYP1A1 induction in murine hepatoma cells (Hepa-1c1c7). Indeed, AOH and AME enhanced the levels of CYP1A1 in Hepa-1c1c7 cells but not in cells with inactivated AhR (Hepa-1c1c12) or ARNT (Hepa-1c1c4). AOH and AME did not increase the production of reactive oxygen species but reduced cell counts in Hepa-1c1c7 cells after 24 and 48 h. This effect, however, was independent of AhR/ARNT. At 48 h, AOH and AME increased apoptosis dependent on AhR and ARNT. In conclusion, AOH and AME are novel inducers of the AhR/ARNT pathway, which mediates induction of CYP1A1 and apoptosis and might thereby contribute to the toxicity of these mycotoxins.
机译:链霉菌霉菌毒素链菌素(AOH)和链霉菌素甲醚(AME)是潜在的致癌物。作为平面化合物,AOH和AME优先被细胞色素P450(CYP)1A1和1A2代谢。 CYP1A1最主要的调节子是二聚体转录因子复合物AhR / ARNT,它被平面配体激活。因此,我们研究了AOH和AME对AhR / ARNT的激活,并监测了小鼠肝癌细胞(Hepa-1c1c7)中的CYP1A1诱导作用。确实,AOH和AME增强了Hepa-1c1c7细胞中CYP1A1的水平,但未增强具有灭活的AhR(Hepa-1c1c12)或ARNT(Hepa-1c1c4)的细胞中的CYP1A1水平。在24和48小时后,AOH和AME不会增加活性氧的产生,但会减少Hepa-1c1c7细胞的细胞计数。但是,此效果独立于AhR / ARNT。在48小时,AOH和AME增加依赖于AhR和ARNT的凋亡。总之,AOH和AME是AhR / ARNT途径的新型诱导剂,其介导CYP1A1的诱导和细胞凋亡,并可能因此对这些真菌毒素的毒性作出贡献。

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