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Increased sialylation of site specific O-glycoforms of hemopexin in liver disease

机译:增加肝病血红素素特异性O-糖族的唾液酸化

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Background: Non-invasive monitoring of liver disease remains an important health issue. Liver secreted glycoproteins reflect pathophysiological states of the organ and represent a rational target for serologic monitoring. In this study, we describe sialylated O-glycoforms of liver-secreted hemopexin (HPX) and quantify them as a ratio of disialylated to monosialylated form (S-HPX). Methods: We measured S-HPX in serum of participants of the HALT-C trial using a LC-MS/MS-MRM assay. Results: Repeated measurements of S-HPX in the samples of 23 disease-free controls, collected at four different time points, show that the ratio remains stable in the healthy controls but increases with the progression of liver disease. The results of measurement of S-HPX in serum of participants of the HALT-C trial show that it increased significantly (Kruskal-Wallis test, p < 0.01) in liver disease as the stage of fibrosis progressed in liver biopsies. We observed a 1.7-fold increase in fibrosis defined as Ishak score 3-4 (24.9 + 14.2, n = 22) and 4.7-fold increase in cirrhosis defined as Ishak score 5-6 (68.6 + 38.5; n = 24) compared to disease-free controls (14.7 + 6.7, n = 23). S-HPX is correlated with AFP, bilirubin, INR, ALT, and AST while inversely correlated with platelet count and albumin. In an independent verification set of samples, S-HPX separated the Ishak 5-6 (n = 15) from the Ishak 3-4 (n = 15) participants with AuROC 0.84; at the same time, the Ishak 3-4 group was separated from disease-free controls (n = 15) with AuROC 0.82. Conclusion: S-HPX, a measure of sialylated O-glycoforms of hemopexin, progressively increases in fibrotic and cirrhotic patient of HCV etiology and can be quantified by an LC-MS/MS-MRM assay in unfractionated serum of patients. Quantification of sialylated O-glycoforms of this liver secreted glycoprotein represents a novel measure of the stage of liver disease that could have a role in monitoring the progression of liver pathology.
机译:背景:肝病的无侵袭性监测仍然是一个重要的健康问题。肝分泌的糖蛋白反射器官的病理生理状态,代表血清学监测的理性靶标。在这项研究中,我们描述了肝分泌的血红蛋白(HPX)的唾液酸化O-糖族,并将它们量化为酸化与单胞苷的形式(S-HPX)的比例。方法:使用LC-MS / MS-MRM测定法测量HALT-C试验的参与者血清中的S-HPX。结果:在四种不同时间点收集的23个无病对照样品中的S-HPX的重复测量,表明,该比率在健康对照中保持稳定,但随着肝病的进展而增加。 HALT-C试验中参与者血清中S-HPX测量结果表明,随着肝脏活组织检查进展的纤维化阶段,它在肝病中增加(Kruskal-Wallis试验,P <0.01)。我们观察到纤维化的增加1.7倍,定义为ISHAK得分3-4(24.9 + 14.2,n = 22)和4.7倍,肝硬化增加,定义为ISHAK得分5-6(68.6 + 38.5; n = 24)无病控制(14.7 + 6.7,n = 23)。 S-HPX与AFP,胆红素,INR,ALT和AST相关联,而AST与血小板计数和白蛋白相反。在一个独立的验证等集中,S-HPX将ISHAK 5-6(n = 15)与AUTOC 0.84的ISHAK 3-4(n = 15)参与者分开;与此同时,ishak 3-4组与Auroc 0.82与无疾病对照(n = 15)分离。结论:S-HPX,血红蛋白唾液酸甘油糖的衡量标准,HCV病因的纤维化和肝硬化患者逐渐增加,可以通过LC-MS / MS-MRM测定在患者的未分割血清中量化。该肝脏分泌的糖蛋白的唾液酸化O-糖蛋白的定量代表了肝脏疾病阶段的新措施,这可能在监测肝脏病理学进展方面具有作用。

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