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Analysis of synthetic cannabinoids using high-resolution mass spectrometry and mass defect filtering: Implications for non-targeted screening of designer drugs

机译:使用高分辨率质谱和大规模缺陷滤波的合成大麻素分析:设计师药物非靶向筛选的影响

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摘要

Detection of new designer drugs remains an analytical challenge due to the ability of manufacturers to rapidly substitute closely related analogs for banned substances. Traditional targeted mass spectrometry methods rely on library searches, known masses, or multiple reaction monitoring (MRM) transitions and are therefore often unable to detect or identify recently discovered or yet unreported designer drug analogs. Here, high-resolution mass spectrometry in conjunction with mass defect filtering is presented as a method for non-targeted analysis to detect both known and novel analogs of designer drugs. The technique is applied in depth to a family of designer drugs composed of indole-derived synthetic cannabinoids closely related to JWH-018, a substance recently controlled in the United States. A single mass defect filter with a 50 mDa window encompasses over 80% of all currently published structures in this family. Searching for precursor ions of common fragment ions enables detection of compounds with mass defects that fall outside the range of mass defect filter parameters. Application of a mass defect filter to fragment ions prior to precursor ion searching increases the breadth of analogs that can be detected. The combined approach defines a broad-spectrum search for related molecules.
机译:由于制造商迅速替代禁用物质的能力,新设计师药物的检测仍然是一个分析挑战。传统的靶向质谱法依赖于图书馆搜索,已知质量或多次反应监测(MRM)转换,因此通常无法检测到或识别最近发现或尚未报告的设计者药物类似物。这里,将高分辨率质谱结合质量缺陷滤波作为非靶向分析的方法,以检测设计者药物的已知和新型类似物。该技术适用于由与JWH-018密切相关的吲哚衍生的合成大麻素组成的设计师药物,该技术应用于与JWH-018密切相关的吲哚衍生的合成大麻素,该物质最近控制在美国。具有50 MDA窗口的单个质量缺陷过滤器包含此系列中当前公布的结构的80%以上。搜索常见碎片离子的前体离子能够检测具有落下的质量缺陷的化合物,该化合物落在质量缺陷过滤器参数范围之外。在前体离子搜索之前将质量缺陷过滤器在片段离子中施加增加,增加了可以检测的类似物的宽度。组合方法定义了对相关分子的广谱搜索。

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