Identifying Metabolites of Meclonazepam by High-Resolution Mass Spectrometry Using Human Liver Microsomes, Hepatocytes, a Mouse Model, and Authentic Urine Samples

被引:0
|
作者
Svante Vikingsson
Ariane Wohlfarth
Mikael Andersson
Henrik Gréen
Markus Roman
Martin Josefsson
Fredrik C Kugelberg
Robert Kronstrand
机构
[1] Linköping University,Clinical Pharmacology, Division of Drug Research, Department of Medical and Health Sciences
[2] National Board of Forensic Medicine,Department of Forensic Genetics and Forensic Toxicology
[3] Linköping University,Department of Physics, Chemistry and Biology
来源
The AAPS Journal | 2017年 / 19卷
关键词
benzodiazepine; metabolism; LC-MS/MS; new psychoactive substance; toxicokinetics;
D O I
暂无
中图分类号
学科分类号
摘要
Meclonazepam is a benzodiazepine patented in 1977 to treat parasitic worms, which recently appeared as a designer benzodiazepine and drug of abuse. The aim of this study was to identify metabolites suitable as biomarkers of drug intake in urine using high-resolution mass spectrometry, authentic urine samples, and different model systems including human liver microsomes, cryopreserved hepatocytes, and a mice model. The main metabolites of meclonazepam found in human urine were amino-meclonazepam and acetamido-meclonazepam; also, minor peaks for meclonazepam were observed in three of four urine samples. These observations are consistent with meclonazepam having a metabolism similar to that of other nitro containing benzodiazepines such as clonazepam, flunitrazepam, and nitrazepam. Both metabolites were produced by the hepatocytes and in the mice model, but the human liver microsomes were only capable of producing minor amounts of the amino metabolite. However, under nitrogen, the amount of amino-meclonazepam produced increased 140 times. This study comprehensively elucidated meclonazepam metabolism and also illustrates that careful selection of in vitro model systems for drug metabolism is needed, always taking into account the expected metabolism of the tested drug.
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页码:736 / 742
页数:6
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