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Qualitative and quantitative analysis of pharmaceutical compounds by MALDI-TOF mass spectrometry.

机译:通过MALDI-TOF质谱对药物化合物进行定性和定量分析。

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摘要

In this report, we discuss key issues for the successful application of MALDI-TOF mass spectrometry to quantify drugs. These include choice and preparation of matrix, nature of cationization agent, automation, and data analysis procedures. The high molecular weight matrix meso-tetrakis(pentafluorophenyl)porphyrin eliminates chemical noise in the low-mass range, a "brushing" spotting technique in combination with prestructured target plates enables fast preparation of homogeneous matrix crystals, and addition of Li+ leads to intense cationized drug species. Complex biological samples were cleaned up using a 96-well solid-phase extraction plate, and the purified samples were automatically spotted by a pipetting robot. To obtain a suitable data analysis procedure for the quantitative analysis of drugs by MALDI-TOF mass spectrometry, various data processing parameters were evaluated on our two model drugs lopinavir and ritonavir. Finally, and most importantly, it is shown that the above-described procedure can be successfully applied to quantify clinically relevant concentrations of lopinavir, an HIV protease inhibitor, in extracts of small numbers of peripheral blood mononuclear cells (1 x 10(6)).
机译:在本报告中,我们讨论了成功应用MALDI-TOF质谱定量药物的关键问题。这些包括基质的选择和制备,阳离子化剂的性质,自动化和数据分析程序。高分子量基体中四(五氟苯基)卟啉消除了低质量范围内的化学噪声,“刷”点技术与预构建的靶板相结合,可以快速制备均质的基体晶体,并且添加Li +会导致强烈的阳离子化药物种类。使用96孔固相萃取板清洁复杂的生物样品,然后通过移液机器人自动点样纯化的样品。为了获得用于通过MALDI-TOF质谱定量分析药物的合适数据分析程序,在我们的两种模型药物lopinavir和ritonavir上评估了各种数据处理参数。最后,最重要的是,已证明上述方法可以成功地用于定量少量外周血单个核细胞提取物中的HIV蛋白酶抑制剂洛匹那韦的临床相关浓度(1 x 10(6)) 。

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