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人肝细胞中新合成大麻素ADB-CHMINACA(MAB-CHMINACA)代谢物的鉴定。

Identification of New Synthetic Cannabinoid ADB-CHMINACA (MAB-CHMINACA) Metabolites in Human Hepatocytes.

作者信息

Carlier Jeremy, Diao Xingxing, Sempio Cristina, Huestis Marilyn A

机构信息

Chemistry & Drug Metabolism Section, Clinical Pharmacology & Therapeutics Research Branch, Intramural Research Program, National Institute on Drug Abuse, National Institutes of Health, Baltimore, Maryland, 21224, USA.

XenoBiotic Laboratories, Inc., Plainsboro, New Jersey, 08536, USA.

出版信息

AAPS J. 2017 Mar;19(2):568-577. doi: 10.1208/s12248-016-0037-5. Epub 2017 Jan 9.

Abstract

ADB-CHMINACA (MAB-CHMINACA) is a new synthetic cannabinoid with high potency and many reported adverse events and fatalities. The drug is currently scheduled in several countries in Europe and the USA. Analytical methods need to be developed to confirm ADB-CHMINACA intake for clinical and forensic programs. For many synthetic cannabinoids, parent compound is not detectable in biological samples after intake, making the detection of metabolites the only way to prove consumption. Therefore, detection of ADB-CHMINACA metabolites in biological specimens is critical. Since there are currently no published data on ADB-CHMINACA metabolism, we aimed to identify its major metabolites. Cryopreserved human hepatocytes were incubated with 10 μmol/L ADB-CHMINACA for 3 h. Incubations were analyzed with liquid chromatography on a biphenyl column, high resolution tandem mass spectrometry (orbitrap), and metabolite identification software. A reference standard of six commercially available potential metabolites was simultaneously analyzed under the same conditions to allow correct assignment of isomers. We detected ten major metabolites. Biotransformations mainly occurred at the cyclohexylmethyl tail of the compound, as also observed with structural analogs' metabolism. Minor reactions also occurred at the tert-butyl chain. Only two analytical standards of potential metabolites matched an actual metabolite detected in hepatocyte incubations. We recommend A9 (ADB-CHMINACA hydroxycyclohexylmethyl), A4 (ADB-CHMINACA 4″-hydroxycyclohexyl), and A6 (ADB-CHMINACA hydroxycyclohexylmethyl) as metabolite targets to document ADB-CHMINACA intake in clinical and forensic cases. Additionally, these results will guide analytical standard manufacturers to better provide suitable references for further studies on ADB-CHMINACA metabolism.

摘要

ADB-CHMINACA(MAB-CHMINACA)是一种新型合成大麻素,效力强劲,有许多关于其不良事件和致死情况的报道。该药物目前在欧洲和美国的多个国家被列入管制。需要开发分析方法,以在临床和法医项目中确认ADB-CHMINACA的摄入情况。对于许多合成大麻素而言,摄入后在生物样本中无法检测到母体化合物,这使得检测代谢物成为证明使用情况的唯一途径。因此,在生物标本中检测ADB-CHMINACA代谢物至关重要。由于目前尚无关于ADB-CHMINACA代谢的公开数据,我们旨在鉴定其主要代谢物。将冷冻保存的人肝细胞与10μmol/L的ADB-CHMINACA孵育3小时。使用联苯柱液相色谱、高分辨率串联质谱(轨道阱)和代谢物鉴定软件对孵育物进行分析。同时在相同条件下分析六种市售潜在代谢物的参考标准品,以正确鉴定异构体。我们检测到了十种主要代谢物。生物转化主要发生在该化合物的环己基甲基尾部,结构类似物的代谢情况也如此。叔丁基链上也发生了少量反应。在肝细胞孵育物中检测到的实际代谢物中,只有两种潜在代谢物的分析标准品与之匹配。我们建议将A9(ADB-CHMINACA羟基环己基甲基)、A4(ADB-CHMINACA 4″-羟基环己基)和A6(ADB-CHMINACA羟基环己基甲基)作为代谢物靶点,用于在临床和法医案件中记录ADB-CHMINACA的摄入情况。此外,这些结果将指导分析标准品制造商更好地为ADB-CHMINACA代谢的进一步研究提供合适的参考。

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