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Performance evaluation of three liquid chromatography mass spectrometry methods for broad spectrum drug screening

机译:三种液相色谱质谱法用于广谱药物筛选的性能评估

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Background: Liquid chromatography-mass spectrometry (LC-MS) and tandem LC-MS (LC-MS/MS) are increasingly used in toxicology laboratories as a complementary method to gas chromatography-mass spectrometry (GC-MS) and liquid chromatography-ultraviolet detection (LC-UV) for comprehensive drug screening (CDS). This study was designed to characterize the sensitivity and specificity of three LC-MS(/MS) vendor-supplied methods for targeted CDS and identify the current limitations associated with the use of these technologies.Methods: Five methods for broad spectrum CDS, including LC-UV (REMEDi), full scan GC-MS, LC-MS (ZQ?-Mass Detector with MassLynx?-software), LC-QTRAP-MS/MS (3200-QTRAP~R with Cliquid~R-software) and LC-LIT-MS/MS (LXQ? Linear Ion Trap with ToxID~TM-software) were evaluated based on their ability to detect drugs in 48 patient urine samples.Results: The tandem MS methods identified 15% more drugs than the single stage MS or LC-UV methods. Use of two broad spectrum screening methods identified more drugs than any single system alone. False negatives and false positives generated by the LC-MS(/MS) software programs were identified upon manual review of the raw data.Conclusions: The LC-MS/MS methods detected a broader menu of drugs; however, it is essential to establish manual data review criteria for all LC-MS(/MS) drug screening methods. Use of an EI-GC-MS and ESI-LC-MS/ MS combination for targeted CDS may be optimal due to the complementary nature of the chromatographic and ionization techniques.
机译:背景:液相色谱-质谱(LC-MS)和串联LC-MS(LC-MS / MS)在毒理学实验室中越来越多地用作气相色谱-质谱(GC-MS)和液相色谱-紫外线的补充方法检测(LC-UV)进行全面的药物筛选(CDS)。这项研究旨在表征针对目标CDS的三种LC-MS(/ MS)供应商提供的方法的敏感性和特异性,并确定与这些技术的使用相关的当前局限。方法:五种广谱CDS方法,包括LC -UV(REMEDi),全扫描GC-MS,LC-MS(带有MassLynx®软件的ZQ?-质谱检测器),LC-QTRAP-MS / MS(带有Cliquid〜R软件的3200-QTRAP〜R)和LC基于LIT-MS / MS(带有ToxID〜TM软件的LXQ?线性离子阱)对48种患者尿液样品中药物的检测能力,进行了评估。结果:串联MS方法比单阶段MS鉴定出的药物多15%或LC-UV方法。使用两种广谱筛查方法比单独使用任何单一系统都能鉴定出更多的药物。手动查看原始数据后,可以识别出LC-MS(/ MS)软件程序生成的假阴性和假阳性结果。结论:LC-MS / MS方法检测到的药物范围更广;但是,必须为所有LC-MS(/ MS)药物筛选方法建立手动数据审查标准。由于色谱和电离技术的互补性,将EI-GC-MS和ESI-LC-MS / MS组合用于目标CDS可能是最佳的。

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