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Mass spectrometry detection of basic drugs in fast chiral analyses with vancomycin stationary phases

机译:万古霉素固定相快速手性分析中基本药物的质谱检测

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摘要

Current trends in chiral analysis of pharmaceutical drugs are focused on faster separations and higher separation efficiencies. Core-shell or superficially porous particles (SPP) based chiral stationary phases (CSPs) provide reduced analysis times while maintaining high column efficiencies and sensitivity. In this study, mobile phase conditions suitable for chiral analyses with electrospray ionization LC-MS were systematically investigated using vancomycin as a representative CSP. The performance of a 2.7 µm SPP based vancomycin CSP (SPP-V) 10 cm × 0.21 cm column was compared to that of a corresponding 5 µm fully porous particles based analogue column. The results demonstrated that the SPP-V column provides higher efficiencies, 2–5 time greater sensitivity and shorter analysis time for a set of 22 basic pharmaceutical drugs. The SPP-V was successfully applied for the analysis of the degradation products of racemic citalopram whose enantiomers could be selectively identified by MS.
机译:药物手性分析的当前趋势集中在更快的分离和更高的分离效率上。基于核壳或表面多孔颗粒(SPP)的手性固定相(CSP)可减少分析时间,同时保持较高的色谱柱效率和灵敏度。在这项研究中,以万古霉素为代表的CSP系统地研究了适合进行电喷雾电离LC-MS手性分析的流动相条件。将2.7µm SPP基万古霉素CSP(SPP-V)10µcm××0.21µcm色谱柱的性能与相应的5µµm全多孔颗粒模拟柱进行了比较。结果表明,对于22种基本药物,SPP-V色谱柱具有更高的效率,高2-5倍的灵敏度和更短的分析时间。 SPP-V成功地用于分析外消旋西酞普兰的降解产物,其对映体可以通过MS进行选择性鉴定。

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