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将红外基质辅助激光解吸电离飞行时间质谱与薄层层析覆盖结合试验相结合及其在追踪肝细胞癌和胰腺癌中肿瘤相关糖鞘脂的临床应用。

Matching IR-MALDI-o-TOF mass spectrometry with the TLC overlay binding assay and its clinical application for tracing tumor-associated glycosphingolipids in hepatocellular and pancreatic cancer.

作者信息

Distler Ute, Hülsewig Marcel, Souady Jamal, Dreisewerd Klaus, Haier Jörg, Senninger Norbert, Friedrich Alexander W, Karch Helge, Hillenkamp Franz, Berkenkamp Stefan, Peter-Katalinić Jasna, Müthing Johannes

机构信息

Institute of Medical Physics and Biophysics and Institute for Hygiene, University of Münster, D-48149 Münster, Germany.

出版信息

Anal Chem. 2008 Mar 15;80(6):1835-46. doi: 10.1021/ac702071x. Epub 2008 Feb 16.

DOI:10.1021/ac702071x
PMID:18278947
Abstract

Glycosphingolipids (GSLs), composed of a hydrophilic carbohydrate chain and a lipophilic ceramide anchor, play pivotal roles in countless biological processes, including the development of cancer. As part of the investigation of the vertebrate glycome, GSL analysis is undergoing rapid expansion owing to the application of modern mass spectrometry. Here we introduce direct coupling of IR-MALDI-o-TOF mass spectrometry with the TLC overlay binding assay for the structural characterization of GSLs. We matched three complementary methods including (i) TLC separation of GSLs, (ii) their detection with oligosaccharide-specific proteins, and (iii) in situ MS analysis of protein-detected GSLs. The high specificity and sensitivity is demonstrated by use of antibodies, bacterial toxins, and a plant lectin. The procedure works on a nanogram scale, and detection limits of less than 1 ng at its best of immunostained GSLs were obtained. Furthermore, only crude lipid extracts of biological sources are required for TLC-IR-MALDI-MS, omitting any laborious GSL downstream purification procedures. This strategy was successfully applied to the identification of cancer-associated GSLs in human hepatocellular and pancreatic tumors. Thus, the in situ TLC-IR-MALDI-MS of immunolabeled GSLs opens new doors by delivering specific structural information of trace quantities of GSLs with only a limited investment in sample preparation.

摘要

糖鞘脂(GSLs)由亲水性碳水化合物链和亲脂性神经酰胺锚组成,在包括癌症发展在内的无数生物过程中发挥着关键作用。作为脊椎动物糖组研究的一部分,由于现代质谱技术的应用,GSL分析正在迅速扩展。在此,我们介绍了红外基质辅助激光解吸电离-串联飞行时间质谱(IR-MALDI-o-TOF MS)与薄层层析(TLC)覆盖结合测定法的直接联用,用于GSLs的结构表征。我们结合了三种互补方法,包括(i)GSLs的TLC分离,(ii)用寡糖特异性蛋白质对其进行检测,以及(iii)对蛋白质检测到的GSLs进行原位质谱分析。通过使用抗体、细菌毒素和植物凝集素证明了该方法具有高特异性和高灵敏度。该方法在纳克级水平上有效,免疫染色的GSLs在最佳情况下检测限低于1纳克。此外,TLC-IR-MALDI-MS仅需要生物来源的粗脂质提取物,无需任何繁琐的GSL下游纯化程序。该策略已成功应用于鉴定人类肝细胞癌和胰腺癌中与癌症相关的GSLs。因此,免疫标记GSLs的原位TLC-IR-MALDI-MS通过仅投入有限的样品制备成本就能提供痕量GSLs的特定结构信息,从而打开了新的大门。

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