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温度和 pH 值依赖性的芬太尼类似物稳定性:降解途径和潜在的生物标志物。

Temperature and pH-dependent stability of fentanyl analogs: Degradation pathways and potential biomarkers.

机构信息

Department of Forensic Science, Sam Houston State University, Huntsville, Texas, USA.

出版信息

J Forensic Sci. 2024 Sep;69(5):1799-1814. doi: 10.1111/1556-4029.15578. Epub 2024 Jul 12.

DOI:10.1111/1556-4029.15578
PMID:38997947
Abstract

The collection, storage, and transport of samples prior to and during analysis is of utmost importance, especially for highly potent analogs that may not be present in high concentrations and are susceptible to pH or thermally mediated degradation. An accelerated stability study was performed on 17 fentanyl analogs (fentalogs) over a wide range of pH (2-10) and temperature (20-60°C) conditions over 24 h. Dilute aqueous systems were used to investigate temperature and pH-dependent kinetics using liquid chromatography-tandem mass spectrometry (LC-MS/MS). Liquid chromatography-quadrupole/time-of-flight-mass spectrometry (LC-Q/TOF-MS) was used for structural elucidation of degradants. With the exception of remifentanil, all fentalogs evaluated were stable at pH 6 or lower. Fentalogs were generally unstable in strongly alkaline environments and at elevated temperatures. Remifentanil was the least stable drug and N-dealkylated fentalogs were the most stable. Fentanyl degraded to acetylfentanyl, norfentanyl, fentanyl N-oxide, and 1-phenethylpyridinium salt (1-PEP). A total of 26 unique breakdown products were observed for 15 of the fentanyl derivatives studied. Common degradation pathways involved N-dealkylation, oxidation of the piperidine nitrogen, and β-elimination of N-phenylpropanamide followed by oxidation/dehydration of the piperidine ring. Ester and amide hydrolysis, demethylation at the propanamide, and O-demethylation were observed for selected fentalogs only. The potential for analyte loss should be considered during the pre-analytical phase (i.e., shipping and transport) where environmental conditions may not be controlled, as well as during the analysis itself.

摘要

在分析之前和期间,样品的收集、存储和运输非常重要,特别是对于可能浓度不高且易受 pH 值或热介导降解影响的高活性类似物。对 17 种芬太尼类似物(芬太尼类似物)在 24 小时内进行了广泛的 pH(2-10)和温度(20-60°C)条件下的加速稳定性研究。使用稀水溶液通过液相色谱-串联质谱(LC-MS/MS)研究温度和 pH 依赖性动力学。使用液相色谱-四极杆/飞行时间质谱(LC-Q/TOF-MS)对降解产物进行结构阐明。除了瑞芬太尼外,评估的所有芬太尼类似物在 pH 6 或更低时都稳定。芬太尼类似物在强碱性环境中和高温下通常不稳定。瑞芬太尼是最不稳定的药物,N-去烷基芬太尼类似物是最稳定的。芬太尼降解为乙酰芬太尼、去甲芬太尼、芬太尼 N-氧化物和 1-苯乙基吡啶盐(1-PEP)。在所研究的 15 种芬太尼衍生物中,共观察到 26 种独特的分解产物。常见的降解途径包括 N-去烷基化、哌啶氮氧化、N-苯丙酰胺的 β-消除,随后哌啶环的氧化/脱水。酯和酰胺水解、丙酰胺的去甲基化以及仅在选定的芬太尼类似物中观察到的 O-去甲基化。在分析之前的阶段(即运输)中,应考虑分析物损失的可能性,因为环境条件可能不受控制,以及在分析本身中。

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