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Quantitative Liquid Chromatography-Mass Spectrometry-Multiple Reaction Monitoring (LC-MS-MRM) analysis of site-specific glycoforms of haptoglobin in liver disease

机译:定量液相色谱-质谱-多反应监测(LC-MS-MRM)分析肝病中触珠蛋白的位点特异性糖型

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Development of liver disease is associated with the appearance of multiply fucosylated glycoforms of haptoglobin. To analyze the disease-related haptoglobin glycoforms in liver cirrhosis and hepatocellular carcinoma, we have optimized an LC-MS-multiple reaction monitoring (MRM) workflow for glycopeptide quantification. The final quantitative analysis included 24 site-specific glycoforms generated by treatment of a tryptic digest of haptoglobin with α(2-3,6,8)-neuraminidase and β(1-4)-galactosidase. The combination of LC-MS-MRM with exoglycosidase digests allowed resolution of isobaric glycoforms of the haptoglobin-T3 glycopeptide for quantification of the multiply fucosylated Lewis Y-containing glycoforms we have identified in the context of liver disease. Fourteen multiply fucosylated glycoforms of the 20 examined increased significantly in the liver disease group compared with healthy controls with an average 5-fold increase in intensity (p < 0.05). At the same time, two tri-antennary glycoforms without fucoses did not increase in the liver disease group, and two tetra-antennary glycoforms without fucoses showed a marginal increase (at most 40%) in intensity. Our analysis of 30 individual patient samples (10 healthy controls, 10 cirrhosis patients, and 10 hepatocellular carcinoma patients) showed that these glycoforms were substantially increased in a small subgroup of liver disease patients but did not significantly differ between the groups of hepatocellular carcinoma and cirrhosis patients. The tri- and tetra-antennary singly fucosylated glycoforms are associated with a MELD score and low platelet counts (p < 0.05). The exoglycosidase-assisted LC-MS-MRM workflow, optimized for the quantification of fucosylated glycoforms of haptoglobin, can be used for quantification of these glycoforms on other glycopeptides with appropriate analytical behavior.
机译:肝病的发展与触珠蛋白的多岩藻糖基化糖形式的出现有关。为了分析肝硬化和肝细胞癌中与疾病相关的触珠蛋白糖型,我们优化了LC-MS-多重反应监测(MRM)工作流程以进行糖肽定量。最终的定量分析包括通过用α(2-3,6,8)-神经氨酸酶和β(1-4)-半乳糖苷酶处理触珠蛋白的胰蛋白酶消化而产生的24种位点特异性糖型。 LC-MS-MRM与糖苷外切酶消化物的组合可分辨触觉球蛋白-T3糖肽的同量糖型,用于定量我们在肝病中鉴定的多重岩藻糖基化的含有路易斯Y的糖型。与健康对照组相比,肝病组中被检查的20种中的14种岩藻糖基化糖型显着增加,强度平均增加5倍(p <0.05)。同时,在肝病组中,没有岩藻糖的两种三触角糖型没有增加,并且两种没有岩藻糖的四触角糖型的强度略有增加(最多40%)。我们对30个患者样本(10个健康对照,10个肝硬化患者和10个肝细胞癌患者)的分析表明,这些糖型在一小部分肝病患者中显着增加,但在肝细胞癌和肝硬化组之间没有显着差异耐心。三触角和四触角岩藻糖基化糖型与MELD评分和低血小板计数相关(p <0.05)。胞外糖苷酶辅助的LC-MS-MRM工作流程经过优化,可量化触珠蛋白的岩藻糖基化糖型,可用于以适当的分析行为对其他糖肽上的这些糖型进行定量。

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