Coulter Cynthia, Gonzales Jonah, Coulter Campbell A, Wagner Jarrad, Moore Christine
9 Delta Analytical, LLC, Ontario, CA 91761, United States.
School of Forensic Sciences, Oklahoma State University Center for Health Sciences, Tulsa, OK 74107, United States.
J Anal Toxicol. 2025 Apr 12;49(4):265-271. doi: 10.1093/jat/bkaf013.
A simple liquid-liquid extraction procedure followed by liquid chromatography-quadrupole time of flight tandem mass spectrometry (LC-QTOF-MS) analysis for drugs in oral fluid collected with the Quantisal™ device has been developed. The decision point cut-off concentrations were at or below those recommended by the National Safety Council's Alcohol, Drugs, and Impairment Division (NSC-ADID) for toxicological investigation of driving under the influence of drugs cases. Currently, the American Acadamy of Forensic Sciences and the Academy Standards Board (ANSI/ASB) Standard 120 does not cover the analysis of oral fluid collected in impaired driving investigations; instead guidance from the NSC-ADID was used. The supporting mass spectral-based screening library was adapted from commercially available databases and included Tier 1 and Tier 2 recommended compounds. Further, the additional inclusion of novel psychoactive substances and synthetic cannabinoids was based on the Center for Forensic Science Research and Education's quarterly publications of 2023. Metabolites from those publications were not included in this method since, with some exceptions, parent drugs are the dominant compounds in oral fluid. Briefly, Quantisal™ (1 mL) was mixed with organic solvents, centrifuged, and decanted; followed by a second liquid-liquid process which extracted all the drugs in a single aliquot. A gradient liquid chromatography program using 0.1% formic acid in water and 0.1% formic acid in methanol was used and the runtime was 10 minutes. LC-QTOF-MS settings were optimized to promote greater sensitivity for a wide range of drug classes. The method was fully validated using ANSI/ASB 036 Standard Practices for Method Validation in Forensic Toxicology as guidance. Interference studies, limit of detection, precision at and around the decision points, ionization suppression/enhancement, and processed sample stability up to 96 hours were completed for each drug in the library database. While ion suppression or enhancement of the analytes varied greatly, the decision point was not significantly affected and internal standards that mimicked similar responses were chosen for each analyte. The method was applied to proficiency program samples, routine samples received in the laboratory, and blind samples screened against the search engine. The optimization of specific tune characteristics and instrument settings allowed the user to meet or exceed recommended screening limits for drugs in Quantisal™ collected oral fluid samples without the need for immunoassay testing.
已开发出一种简单的液-液萃取程序,随后采用液相色谱-四极杆飞行时间串联质谱(LC-QTOF-MS)分析法对使用Quantisal™装置采集的口腔液中的药物进行分析。判定点截止浓度等于或低于美国国家安全委员会酒精、药物与损伤司(NSC-ADID)针对药物影响下驾驶毒理学调查所推荐的浓度。目前,美国法医科学学会和学会标准委员会(ANSI/ASB)标准120未涵盖在驾驶能力受损调查中采集的口腔液分析;取而代之的是采用了NSC-ADID的指导意见。基于质谱的支持性筛查库改编自市售数据库,包括1级和2级推荐化合物。此外,新型精神活性物质和合成大麻素的额外纳入是基于法医科学研究与教育中心2023年的季度出版物。这些出版物中的代谢物未包含在本方法中,因为除了一些例外情况,母体药物是口腔液中的主要化合物。简要地说,将Quantisal™(1 mL)与有机溶剂混合,离心并倾析;接着进行第二次液-液处理,从单个等分试样中萃取所有药物。使用在水中含0.1%甲酸和在甲醇中含0.1%甲酸的梯度液相色谱程序,运行时间为10分钟。对LC-QTOF-MS设置进行了优化,以提高对多种药物类别的灵敏度。该方法以ANSI/ASB 036《法医毒理学方法验证标准操作规程》为指导进行了全面验证。针对库数据库中的每种药物,完成了干扰研究、检测限、判定点及附近的精密度、电离抑制/增强以及处理后样品长达96小时的稳定性研究。虽然分析物的离子抑制或增强差异很大,但判定点未受到显著影响,并且为每种分析物选择了模拟相似响应的内标。该方法应用于能力验证计划样品、实验室收到的常规样品以及针对搜索引擎筛查的盲样。特定调谐特性和仪器设置的优化使用户能够在无需免疫分析测试的情况下,达到或超过针对使用Quantisal™采集的口腔液样品中药物的推荐筛查限值。
