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Induction and repression effects on CYP and transporter protein abundance by azole mixture uptake in rat liver

机译:丙唑混合物在大鼠肝脏上吸收对CYP和转运蛋白丰度的诱导和抑制作用

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摘要

Detection of mixture effects is a major challenge in current experimental and regulatory toxicology. Robust markers are needed that are easy to quantify and responsive to chemical stressors in a broad dose range. Several hepatic enzymes and proteins related to drug metabolism like cytochrome-P-450 (CYP) enzymes and transporters have been shown to be responsive to pesticide active substances in a broad dose range and are therefore good candidates to be used as markers for mixture toxicity. Even though they can be well quantified at the mRNA level, quantification on the protein level is challenging because most of these proteins are membrane bound. Here we report the development of mass spectrometry-based assays using triple-x-proteomics (TXP) antibodies in combination with targeted selected ion monitoring (tSIM) to quantify changes of protein levels due to exposure to mixtures of pesticide active substances. Our results indicate that changes on the protein level of CYP1A1, ABCB2, ABCC3 are in line with observations on the mRNA and enzyme activity level and are indicative of mixture effects. Therefore, the tests are promising to reveal effects by chemical mixture effects in toxicological studies in rats.
机译:检测混合效应是目前实验和调节毒理学中的主要挑战。需要鲁棒标记,这易于量化和响应于宽剂量范围内的化学压力。已经显示出与药物代谢相关的几种肝脏酶和蛋白质,如细胞色素-P-450(CYP)和转运蛋白有响应于宽剂量范围内的农药活性物质,因此是用作混合物毒性的标志物的良好候选物。即使它们可以在mRNA水平上量化,蛋白质水平的定量也是具有挑战性,因为大多数这些蛋白质是膜结合。在这里,我们通过与靶向所选离子监测(TSIM)组合的三X-蛋白质组学(TXP)抗体来报告基于质谱的基于基于质谱的测定的开发,以定量由于农药活性物质的混合物暴露而定量蛋白质水平的变化。我们的结果表明,CYP1A1,ABCB2,ABCC3的蛋白质水平的变化符合对mRNA和酶活性水平的观察结果,并指示混合效应。因此,该试验令人欣然存在于大鼠毒理学研究中的化学混合物作用揭示效果。

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