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液质萃取表面分析质谱法(LESA-MS)作为一种新型的药物分布和代谢分析工具:特非那定实例。

Liquid extraction surface analysis mass spectrometry (LESA-MS) as a novel profiling tool for drug distribution and metabolism analysis: the terfenadine example.

机构信息

Advion Inc., Ithaca, NY 14850, USA.

出版信息

Rapid Commun Mass Spectrom. 2011 Dec 15;25(23):3587-96. doi: 10.1002/rcm.5274.

DOI:10.1002/rcm.5274
PMID:22095508
Abstract

Liquid extraction surface analysis mass spectrometry (LESA-MS) is a novel surface profiling technique that combines micro-liquid extraction from a solid surface with nano-electrospray mass spectrometry. One potential application is the examination of the distribution of drugs and their metabolites by analyzing ex vivo tissue sections, an area where quantitative whole body autoradiography (QWBA) is traditionally employed. However, QWBA relies on the use of radiolabeled drugs and is limited to total radioactivity measured whereas LESA-MS can provide drug- and metabolite-specific distribution information. Here, we evaluate LESA-MS, examining the distribution and biotransformation of unlabeled terfenadine in mice and compare our findings to QWBA, whole tissue LC/MS/MS and MALDI-MSI. The spatial resolution of LESA-MS can be optimized to ca. 1 mm on tissues such as brain, liver and kidney, also enabling drug profiling within a single organ. LESA-MS can readily identify the biotransformation of terfenadine to its major, active metabolite fexofenadine. Relative quantification can confirm the rapid absorption of terfendine after oral dosage, its extensive first pass metabolism and the distribution of both compounds into systemic tissues such as muscle, spleen and kidney. The elimination appears to be consistent with biliary excretion and only trace levels of fexofenadine could be confirmed in brain. We found LESA-MS to be more informative in terms of drug distribution than a comparable MALDI-MS imaging study, likely due to its favorable overall sensitivity due to the larger surface area sampled. LESA-MS appears to be a useful new profiling tool for examining the distribution of drugs and their metabolites in tissue sections.

摘要

液相微萃取表面分析质谱法(LESA-MS)是一种新型的表面分析技术,它结合了从固体表面进行微液萃取和纳喷雾质谱分析。其潜在应用之一是通过分析离体组织切片来检测药物及其代谢物的分布,这是传统上定量全身放射自显影术(QWBA)的应用领域。然而,QWBA 依赖于放射性标记药物的使用,并且仅限于测量总放射性,而 LESA-MS 可以提供药物和代谢物特异性的分布信息。在这里,我们评估了 LESA-MS,考察了未标记特非那定在小鼠中的分布和生物转化,并将我们的发现与 QWBA、全组织 LC/MS/MS 和 MALDI-MSI 进行了比较。LESA-MS 的空间分辨率可以在脑、肝和肾等组织上优化到约 1mm,还可以在单个器官内进行药物分析。LESA-MS 可以轻松识别特非那定向其主要的活性代谢物非索非那定的生物转化。相对定量可以确认口服剂量后特非那定的快速吸收、其广泛的首过代谢以及两种化合物在肌肉、脾脏和肾脏等系统组织中的分布。消除似乎与胆汁排泄一致,并且仅在脑中确认到痕量的非索非那定。与可比的 MALDI-MS 成像研究相比,LESA-MS 在药物分布方面提供了更多信息,这可能是由于其更大的表面积采样导致的整体灵敏度较高。LESA-MS 似乎是一种用于检查组织切片中药物及其代谢物分布的有用的新分析工具。

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