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Analysis of AMB-FUBINACA Biotransformation Pathways in Human Liver Microsome and Zebrafish Systems by Liquid Chromatography-High Resolution Mass Spectrometry

机译:液相色谱-高分辨率质谱法分析人肝微粒体和斑马鱼系统中AMB-FUBINACA的生物转化途径

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摘要

In this study, the metabolic profiles of a new illicit drug AMB-FUBINACA were investigated using both human liver microsome and zebrafish models. Liquid chromatography Q Extractive HF Hybrid Quadrupole-Orbitrap mass spectrometry (LC-QE-HF-MS) was employed to analyze the metabolic sites and pathways. AMB-FUBINACA was added to the in vitro liver microsome incubation model to simulate the metabolic processes in human body. The results showed that a total of 17 metabolites were generated in the human liver microsome model; the main metabolic pathways of the phase I metabolism included ester hydrolysis, methylation, ester hydrolysis combined with decarboxylation, hydroxylation, ester hydrolysis combined with indazole ring hydroxylation, etc. while glucuronidation served as the main metabolic pathway of the phase II metabolism. The zebrafish system produced a similar result with 16 of the same 17 metabolites identified. The phase I metabolites M3.1 (ester hydrolysis), M1.2 (alkyl chain hydrolysis) and the phase II metabolite M3.2 (M3.1 glucuronide) were recommended to be the potential poisoning markers.
机译:在这项研究中,使用人肝微粒体和斑马鱼模型研究了一种新的非法药物AMB-FUBINACA的代谢特征。液相色谱Q萃取HF混合四极杆Orbitrap质谱(LC-QE-HF-MS)用于分析代谢部位和途径。将AMB-FUBINACA添加到体外肝微粒体温育模型中,以模拟人体的代谢过程。结果表明,在人肝微粒体模型中总共产生了17种代谢物。 I期代谢的主要代谢途径包括酯水解,甲基化,酯水解与脱羧结合,羟基化,酯水解与吲唑环羟基化结合等,而葡糖醛酸化作用是II期代谢的主要代谢途径。斑马鱼系统产生了相似的结果,其中鉴定出17种相同的代谢产物中的16种。建议将I相代谢物M3.1(酯水解),M1.2(烷基链水解)和II相代谢物M3.2(M3.1葡糖醛酸)作为潜在的中毒标志物。

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