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首页> 外文期刊>Drug testing and analysis >Metabolic profiling of synthetic cannabinoid 5F-ADB by human liver microsome incubations and urine samples using high-resolution mass spectrometry
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Metabolic profiling of synthetic cannabinoid 5F-ADB by human liver microsome incubations and urine samples using high-resolution mass spectrometry

机译:使用高分辨率质谱法通过人肝微粒孵育和尿液样品的合成大麻素5F-adb的代谢分析

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摘要

5F-ADB (methyl 2-{[1-(5-fluoropentyl)-1H-indazole-3-carbonyl] amino}-3,3-dimethylbutanoate) is a frequently abused new synthetic cannabinoid that has been sold since at least the end of 2014 on the drug market and has been classified as an illicit drug in most European countries, as well as Turkey, Japan, and the United States. In this study, the in vitro metabolism of 5F-ADB was investigated by using pooled human liver microsomes (HLMs) assay and liquid chromatography-high-resolution mass spectrometry (LC-HRMS). 5F-ADB (5 mu mol/L) was incubated with HLMs for up to 3 hours, and the metabolites were identified using LC-HRMS and software-assisted data mining. The in vivo metabolism was investigated by the analysis of 30 authentic urine samples and was compared to the data received from the in vitro metabolism study. Less than 3.3% of the 5F-ADB parent compound remained after 1 hour of incubation, and no parent drug was detected after 3 hours. We identified 20 metabolites formed via ester hydrolysis, N-dealkylation, oxidative defluorination, hydroxylation, dehydrogenation, further oxidation to N-pentanoic acid and glucuronidation or a combination of these reactions in vitro. In 12 urine samples (n = 30), 5F-ADB was detected as the parent drug. Three of the identified main metabolites 5F-ADB carboxylic acid (M20), monohydroxypentyl-5F-ADB (M17), and carboxypentyl ADB carboxylic acid (M8) were suggested as suitable urinary markers. The screening of 8235 authentic urine samples for identified 5F-ADB metabolites in vitro resulted in 3135 cases of confirmed 5F-ADB consumption (38%).
机译:5F-ADB(甲基2 - {[1-(5-氟戊基)-1H-吲唑-3-羰基]氨基} -3,3-二甲基丁酸酯)是常用的新合成大麻素,其自至少结束以来已出售2014年在毒品市场上,已被归类为大多数欧洲国家的非法药物,以及土耳其,日本和美国。在该研究中,通过使用汇集的人肝微粒体(HLMS)测定和液相色谱 - 高分辨率质谱(LC-HRMS)来研究5F-ADB的体外代谢。将5F-ADB(5μmol/ L)与HLM一起温育长达3小时,并使用LC-HRMS和软件辅助数据挖掘鉴定代谢物。通过分析30个正宗的尿液样本来研究体内代谢,并与来自体外代谢研究的数据进行比较。在孵育1小时后,少于3F-ADB母体化合物的3.3%,并且在3小时后没有检测到母体药物。我们鉴定了通过酯水解,N-Deafkylation,氧化偏荧光,羟基化,脱氢,对正戊酸和葡糖醛酸的进一步氧化或在体外的组合形成20代谢物。在12个尿液样品(n = 30)中,检测5f-adb作为母体药物。提出了三种鉴定的主要代谢物5F-ADB羧酸(M20),单羟基戊基-5F-ADB(M17)和羧烯醇亚甲基羧酸(M8)作为合适的尿标记。用于鉴定的5F-ADB代谢物的8235正宗尿液样品的筛选导致3135例确诊的5F-ADB消耗(38%)。

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