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Revisiting the Metabolism and Bioactivation of Ketoconazole in Human and Mouse Using Liquid Chromatography–Mass Spectrometry-Based Metabolomics

机译:使用液相色谱-质谱联用的代谢组学研究酮康唑在人和小鼠中的代谢和生物活化

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摘要

Although ketoconazole (KCZ) has been used worldwide for 30 years, its metabolic characteristics are poorly described. Moreover, the hepatotoxicity of KCZ limits its therapeutic use. In this study, we used liquid chromatography–mass spectrometry-based metabolomics to evaluate the metabolic profile of KCZ in mouse and human and identify the mechanisms underlying its hepatotoxicity. A total of 28 metabolites of KCZ, 11 of which were novel, were identified in this study. Newly identified metabolites were classified into three categories according to the metabolic positions of a piperazine ring, imidazole ring, and N-acetyl moiety. The metabolic characteristics of KCZ in human were comparable to those in mouse. Moreover, three cyanide adducts of KCZ were identified in mouse and human liver microsomal incubates as “flags” to trigger additional toxicity study. The oxidation of piperazine into iminium ion is suggested as a biotransformation responsible for bioactivation. In summary, the metabolic characteristics of KCZ, including reactive metabolites, were comprehensively understood using a metabolomics approach.
机译:尽管酮康唑(KCZ)在世界范围内已使用30年,但其代谢特性却鲜为人知。此外,KCZ的肝毒性限制了其治疗用途。在这项研究中,我们使用了基于液相色谱-质谱的代谢组学来评估KCZ在小鼠和人体内的代谢谱,并确定其肝毒性的潜在机制。在这项研究中,共鉴定出28种KCZ代谢物,其中11种是新的。根据哌嗪环,咪唑环和N-乙酰基的代谢位置,新近鉴定的代谢物可分为三类。人体内KCZ的代谢特征与小鼠相当。此外,在小鼠和人肝微粒体培养物中鉴定出KCZ的三种氰化物加合物是“标志”,以引发其他毒性研究。建议将哌嗪氧化成亚胺离子是负责生物活化的生物转化。总之,使用代谢组学方法可以全面了解KCZ的代谢特征,包括反应性代谢物。

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