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通过与人肝微粒体孵育及超高效液相色谱-高分辨质谱法研究合成大麻素受体激动剂PX-1(5F-APP-PICA)的I相代谢

Phase I metabolism of synthetic cannabinoid receptor agonist PX-1 (5F-APP-PICA) via incubation with human liver microsomes and UHPLC-HRMS.

作者信息

Presley Brandon C, Logan Barry K, Jansen-Varnum Susan A

机构信息

Department of Chemistry, Temple University, Philadelphia, PA, USA.

The Center for Forensic Science Research and Education at the Fredric Rieders Family Foundation, Willow Grove, PA, USA.

出版信息

Biomed Chromatogr. 2020 Mar;34(3):e4786. doi: 10.1002/bmc.4786. Epub 2020 Jan 9.

DOI:10.1002/bmc.4786
PMID:31863591
Abstract

Studies of the metabolic and pharmacological profiles of indole carboxamide synthetic cannabinoids (a prevalent class of new psychoactive substances) are critical in ensuring that their use can be detected through bioanalytical testing. We have determined the in vitro Phase I metabolism of one such compound, PX-1 (5F-APP-PICA), and appropriate markers to demonstrate human consumption. PX-1 was incubated with human liver microsomes, followed by analysis of the extracts via high-resolution mass spectrometry. A total of 10 metabolites were identified, with simultaneous defluorination and monohydroxylation of the pentyl side chain as the primary biotransformation product (M1). Additional metabolites formed were hydroxylation products of the indole and benzyl moieties, distal amide hydrolysis, N-desfluoropentyl, and carboxypentyl metabolites. Three monohydroxylated metabolites specific to PX-1 were identified and are reported for the first time in this study. The primary metabolite, M1, was further oxidized to M5, a carboxypentyl metabolite. M8 is PX-1 specific, possessing an intact fluoropentyl side chain. These three metabolites are the most suitable for implementation into bioanalytical assays for demonstrating PX-1 consumption. The findings of this study can be used by analytical scientists and medical professionals to determine PX-1 ingestion and predict the metabolites of synthetic cannabinoids sharing structural elements.

摘要

对吲哚羧酰胺合成大麻素(一类常见的新型精神活性物质)的代谢和药理特性进行研究,对于确保能够通过生物分析检测来发现其使用情况至关重要。我们已经确定了一种此类化合物PX-1(5F-APP-PICA)的体外I相代谢情况以及用于证明人体摄入的合适标志物。将PX-1与人肝微粒体一起孵育,然后通过高分辨率质谱对提取物进行分析。总共鉴定出10种代谢物,戊基侧链同时脱氟和单羟基化作为主要生物转化产物(M1)。形成的其他代谢物是吲哚和苄基部分的羟基化产物、远端酰胺水解产物、N-去氟戊基和羧基戊基代谢物。鉴定出了三种PX-1特有的单羟基化代谢物,本研究首次对其进行报道。主要代谢物M1进一步氧化为M5,一种羧基戊基代谢物。M8是PX-1特有的,具有完整的氟戊基侧链。这三种代谢物最适合用于生物分析检测以证明PX-1的摄入情况。分析科学家和医学专业人员可以利用本研究的结果来确定PX-1的摄入情况,并预测具有相同结构元素的合成大麻素的代谢物。

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