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Analyzing complex mixtures of drug-like molecules: ion mobility as an adjunct to existing liquid chromatography-(tandem) mass spectrometry methods

机译:分析药物样分子的复杂混合物:离子迁移率作为现有液相色谱 - (串联)质谱法的辅助手段

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摘要

The use of traveling wave ion mobility mass spectrometry (TWIMS) is evaluated in conjunction with, and as a possible alternative to, conventional LC-MS(/MS) methods for the separation and characterization of drug-like compounds and metabolites. As a model system we use an in vitro incubation mixture of the chemotherapeutic agent melphalan, which results in more than ten closely related hydrolysis products and chain-like oligomers. Ion mobility as a filtering tool results in the separation of ions of interest from interfering ions, based on charge state and shape/size. Different classes of chemical compounds often display different mobilities even if they show the same LC behavior – thereby providing an orthogonal separation dimension. Small molecules with identical or similar m/z that only differ in shape/size (e.g. isomers and isobars, monomers/dimers) can also be distinguished using ion mobility. Similar to retention times and mass-to-charge ratios, drift times are analyte-dependent and can be used as an additional identifier. We find that the compound melphalan shows two different drift times due to the formation of gas-phase charge isomers (protomers). The occurrence of protomers has important implications for ion mobility characterization of such analytes, and also for the interpretation of their fragmentation behavior (CID) in the gas phase.
机译:结合传统的LC-MS(/ MS)方法(用于分离和表征类药物化合物和代谢物),评估了行波离子淌度质谱(TWIMS)的使用,并可能替代这种方法。作为模型系统,我们使用化学治疗剂美法仑的体外培养混合物,可产生十多种密切相关的水解产物和链状低聚物。离子迁移率作为一种过滤工具,可根据电荷状态和形状/大小将目标离子与干扰离子分离。即使不同类别的化合物表现出相同的LC行为,它们通常也会显示出不同的迁移率,从而提供了正交的分离尺寸。 m / z相同或相似但形状/大小不同的小分子(例如异构体和等压线,单体/二聚体)也可以使用离子迁移率进行区分。与保留时间和质荷比相似,漂移时间与分析物有关,可以用作附加标识。我们发现,由于气相电荷异构体(protomer)的形成,化合物美法仑显示出两个不同的漂移时间。准分子的出现对此类分析物的离子迁移率表征以及在气相中其裂解行为(CID)的解释都具有重要意义。

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