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使用液相色谱- Q Exactive - HF混合四极杆-轨道阱质谱(LC - QE - HF - MS)对真实人类尿液样本中的新型氟硝西泮代谢物进行表征和初步鉴定。

Characterization and tentative identification of new flunitrazepam metabolites in authentic human urine specimens using liquid chromatography-Q exactive-HF hybrid quadrupole-Orbitrap-mass spectrometry (LC-QE-HF-MS).

作者信息

Qin Shiyang, Xin Guobin, Wang Yuanfeng, Qiao Jing, Zhang Wenfang, Xu Duoqi, Xu Zizhen, Liu Yongtao, Zhang Ying, Lu Jianghai

机构信息

Key Laboratory of Forensic Toxicology, Ministry of Public Security, The Criminal Investigation Department of Beijing Public Security Bureau, Beijing, 100085, China.

Key Laboratory of Evidence Science, China University of Political Science and Law, 100025, Beijing, China.

出版信息

J Mass Spectrom. 2019 Aug;54(8):704-715. doi: 10.1002/jms.4383.

DOI:10.1002/jms.4383
PMID:31233253
Abstract

Flunitrazepam (FNZ) is a potent hypnotic, sedative, and amnestic drug used to treat severe insomnia. In our recent study, FNZ metabolic profiles were investigated carefully. Six authentic human urine samples were purified using solid phase extraction (SPE) without enzymatic hydrolysis, and urine extracts were then analyzed by liquid chromatography-Q exactive-HF hybrid quadrupole-Orbitrap-mass spectrometry (LC-QE-HF-MS), using the full scan positive ion mode and targeted MS/MS (ddms2) technique to make accurate mass measurements. There were 25 metabolites, including 13 phase I and 12 phase II metabolites, which were detected and tentatively identified by LC-QE-HF-MS. In addition, nine previously unreported phase II glucuronide conjugates and four phase I metabolites are reported here for the first time. Eight metabolic pathways, including N-reduction and O-reduction, N-glucuronidation, O-glucuronidation, mono-hydroxylation and di-hydroxylation, demethylation, acetylation, and combinations, were implicated in this work, and 2-O-reduction together with dihydroxylation were two novel metabolic pathways for FNZ that were identified tentatively. Although 7-amino FNZ is widely considered to be the primary metabolite, a previously unreported metabolites (M12) can also serve as a potential biomarker for FNZ misuse.

摘要

氟硝西泮(FNZ)是一种强效催眠、镇静和失忆药物,用于治疗严重失眠。在我们最近的研究中,对FNZ的代谢谱进行了仔细研究。使用固相萃取(SPE)对六个真实的人尿液样本进行纯化,无需酶水解,然后通过液相色谱-Q精确-HF混合四极杆-轨道阱质谱(LC-QE-HF-MS)对尿液提取物进行分析,采用全扫描正离子模式和靶向MS/MS(ddms2)技术进行精确质量测量。共检测到25种代谢物,包括13种I相代谢物和12种II相代谢物,并通过LC-QE-HF-MS进行了初步鉴定。此外,本文首次报道了9种以前未报道的II相葡萄糖醛酸共轭物和4种I相代谢物。本研究涉及8种代谢途径,包括N-还原和O-还原、N-葡萄糖醛酸化、O-葡萄糖醛酸化、单羟基化和二羟基化、去甲基化、乙酰化以及它们的组合,其中2-O-还原和二羟基化是初步鉴定出的FNZ的两种新代谢途径。尽管7-氨基FNZ被广泛认为是主要代谢物,但一种以前未报道的代谢物(M12)也可作为FNZ滥用的潜在生物标志物。

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