首页> 外文期刊>Drug testing and analysis >Lefetamine-derived designer drugs N-ethyl-1,2-diphenylethylamine (NEDPA) and N-iso-propyl-1,2-diphenylethylamine (NPDPA): Metabolism and detectability in rat urine using GC-MS, LC-MS(n) and LC-HR-MS/MS.
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Lefetamine-derived designer drugs N-ethyl-1,2-diphenylethylamine (NEDPA) and N-iso-propyl-1,2-diphenylethylamine (NPDPA): Metabolism and detectability in rat urine using GC-MS, LC-MS(n) and LC-HR-MS/MS.

机译:源自左苯丙胺的设计药物N-乙基1,2-二苯乙胺(NEDPA)和N-异丙基1,2-二苯乙胺(NPDPA):使用GC-MS,LC-MS(n)在大鼠尿液中的代谢和可检测性和LC-HR-MS / MS。

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N-Ethyl-1,2-diphenylethylamine (NEDPA) and N-iso-propyl-1,2-diphenylethylamine (NPDPA) are two designer drugs, which were confiscated in Germany in 2008. Lefetamine (N,N-dimethyl-1,2-diphenylethylamine, also named L-SPA), the pharmaceutical lead of these designer drugs, is a controlled substance in many countries. The aim of the present work was to study the phase I and phase II metabolism of these drugs in rats and to check for their detectability in urine using the authors' standard urine screening approaches (SUSA). For the elucidation of the metabolism, rat urine samples were worked up with and without enzymatic cleavage, separated and analyzed by gas chromatography-mass spectrometry (GC-MS) and liquid chromatography-high resolution-tandem mass spectrometry (LC-HR-MS/MS). According to the identified metabolites, the following metabolic pathways for NEDPA and NPDPA could be proposed: N-dealkylation, mono- and bis-hydroxylation of the benzyl ring followed by methylation of one of the two hydroxy groups, combinations of these steps, hydroxylation of the phenyl ring after N-dealkylation, glucuronidation and sulfation of all hydroxylated metabolites. Application of a 0.3 mg/kg BW dose of NEDPA or NPDPA, corresponding to a common lefetamine single dose, could be monitored in rat urine using the authors' GC-MS and LC-MS(n) SUSA. However, only the metabolites could be detected, namely N-deethyl-NEDPA, N-deethyl-hydroxy-NEDPA, hydroxy-NEDPA, and hydroxy-methoxy-NEDPA or N-de-iso-propyl-NPDPA, N-de-iso-propyl-hydroxy-NPDPA, and hydroxy-NPDPA. Assuming similar kinetics, an intake of these drugs should also be detectable in human urine. Copyright ? 2014 John Wiley & Sons, Ltd.
机译:N-乙基1,2-二苯乙胺(NEDPA)和N-异丙基1,2-二苯乙胺(NPDPA)是两种名牌药物,于2008年在德国被没收。左苯丙胺(N,N-二甲基-1,这些设计药物的药物领先者2-二苯乙胺(也称为L-SPA)在许多国家/地区是受控物质。本工作的目的是研究这些药物在大鼠中的I期和II期代谢,并使用作者的标准尿液筛查方法(SUSA)检查其在尿液中的可检测性。为了阐明新陈代谢,对大鼠尿液样品进行了酶裂解处理和不进行酶裂解处理,并通过气相色谱-质谱(GC-MS)和液相色谱-高分辨率串联质谱(LC-HR-MS /多发性硬化症)。根据鉴定出的代谢物,可以提出以下针对NEDPA和NPDPA的代谢途径:N-脱烷基化,苄基环的单-和双-羟基化,随后两个羟基之一的甲基化,这些步骤的组合,所有羟基化代谢物经过N-脱烷基,葡糖醛酸化和硫酸化后的苯环可以使用作者的GC-MS和LC-MS(n)SUSA在大鼠尿液中监测0.3 mg / kg BW剂量的NEDPA或NPDPA的使用,相当于普通的Lefetamine单剂量。但是,只能检测到代谢物,即N-去乙基-NEDPA,N-去乙基-羟基-NEDPA,羟基-NEDPA和羟基-甲氧基-NEDPA或N-去-异丙基-NPDPA,N-去-异-丙基-羟基-NPDPA和羟基-NPDPA。假设动力学相似,在人尿中也应可检测到这些药物的摄入。版权? 2014 John Wiley&Sons,Ltd.

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