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DOI10.1002/dta.1865
In vitro characterization of potential CYP- and UGT-derived metabolites of the psychoactive drug 25B-NBOMe using LC-high resolution MS
Boumrah, Yacine1,2; Humbert, Luc3; Phanithavong, Melodie3; Khimeche, Kamel4; Dahmani, Abdallah1; Allorge, Delphine3,5
通讯作者Boumrah, Yacine
来源期刊DRUG TESTING AND ANALYSIS
ISSN1942-7603
EISSN1942-7611
出版年2016
卷号8期号:2页码:248-256
英文摘要

One of the main challenges posed by the emergence of new psychoactive substances is their identification in human biological samples. Trying to detect the parent drug could lead to false-negative results when the delay between consumption and sampling has been too long. The identification of their metabolites could then improve their detection window in biological matrices. Oxidative metabolism by cytochromes P450 and glucuronidation are two major detoxification pathways in humans. In order to characterize possible CYP- and UGT-dependent metabolites of the 2-(4-bromo-2,5-dimethoxy-phenyl)-N-[(2-methoxyphenyl)methyl]ethanamine (25B-NBOMe), a synthetic psychoactive drug, analyses of human liver microsome (HLM) incubates were performed using an ultra-high performance liquid chromatography system coupled with a quadrupole-time of flight mass spectrometry detector (UHPLC-Q-TOF/MS). On-line analyses were performed using a Waters OASIS HLB column (30 x 2.1 mm, 20 mu m) for the automatic sample loading and a Waters ACQUITY HSS C18 column (150 x 2 mm, 1.8 mu m) for the chromatographic separation. Twenty-one metabolites, consisting of 12 CYP-derived and 9 UGT-derived metabolites, were identified. O-Desmethyl metabolites were the most abundant compounds after the phase I process, which appears to be in accordance with data from previously published NBOMe-intoxication case reports. Although other important metabolic transformations, such as sulfation, acetylation, methylation or glutathione conjugation, were not studied and artefactual metabolites might have been produced during the HLM incubation process, the record of all the metabolite MS spectra in our library should enable us to characterize relevant metabolites of 25B-NBOMe and allow us to detect 25B-MBOMe users. Copyright (c) 2015 John Wiley & Sons, Ltd.


英文关键词metabolism human liver microsomes 25B-NBOMe in vitro UHPLC-Q-TOF MS
类型Article
语种英语
国家Algeria ; France
收录类别SCI-E
WOS记录号WOS:000370199000013
WOS关键词LIQUID-CHROMATOGRAPHY ; HUMAN HEPATOCYTES ; EMERGING DRUGS ; DESIGNER DRUGS ; LEGAL HIGHS ; ION-TRAP ; SUBSTANCES ; ABUSE ; RATS
WOS类目Biochemical Research Methods ; Chemistry, Analytical ; Pharmacology & Pharmacy
WOS研究方向Biochemistry & Molecular Biology ; Chemistry ; Pharmacology & Pharmacy
资源类型期刊论文
条目标识符http://119.78.100.177/qdio/handle/2XILL650/192277
作者单位1.USTHB, Fac Chim, Lab Thermodynam & Modelisat Mol, BP 32 El Alia, Bab Ezzouar 16111, Alger, Algeria;
2.Inst Natl Criminalist & Criminol INCC GN, Bouchaoui, Alger, Algeria;
3.CHRU Lille, Toxicol Lab, Pole Biol Pathol Genet, Bd Prof J Leclercq, F-59037 Lille, France;
4.Ecole Mil Polytech EMP, BP 17 Bordj El Bahri, Algiers, Algeria;
5.Univ Lille 2, EA4483, F-59045 Lille, France
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Boumrah, Yacine,Humbert, Luc,Phanithavong, Melodie,et al. In vitro characterization of potential CYP- and UGT-derived metabolites of the psychoactive drug 25B-NBOMe using LC-high resolution MS[J],2016,8(2):248-256.
APA Boumrah, Yacine,Humbert, Luc,Phanithavong, Melodie,Khimeche, Kamel,Dahmani, Abdallah,&Allorge, Delphine.(2016).In vitro characterization of potential CYP- and UGT-derived metabolites of the psychoactive drug 25B-NBOMe using LC-high resolution MS.DRUG TESTING AND ANALYSIS,8(2),248-256.
MLA Boumrah, Yacine,et al."In vitro characterization of potential CYP- and UGT-derived metabolites of the psychoactive drug 25B-NBOMe using LC-high resolution MS".DRUG TESTING AND ANALYSIS 8.2(2016):248-256.
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