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Revisiting the Metabolism of Ketoconazole Using Accurate Mass

机译:使用精确质量重新研究酮康唑的代谢

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The microsomal metabolism of ketoconazole is revisited using accurate mass LC/MSn and deuterium labelling. Structures for sixteen metabolites are proposed from rat and human microsomal metabolism of commercial ketoconazole. Thirteen of the proposed structures are well determined and consistent with all data; five of the proposed structures are less certain. Ten of the metabolites are described for the first time. Reaction phenotyping shows that most of the metabolites arise from CYP3A4, the enzyme known to be well inhibited by ketoconazole.
机译:使用精确的质量LC / MSn和氘标记技术重新审视了酮康唑的微粒体代谢。从大鼠和人的商业酮康唑的微粒体代谢中提出了十六种代谢物的结构。拟议的结构中有十三项已确定并与所有数据保持一致;提议的结构中有五个尚不确定。首次描述了十种代谢物。反应表型表明,大多数代谢物均来自CYP3A4,该酶被酮康唑很好地抑制。

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