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首页> 外文期刊>Proteomics. Clinical applications >Immunoglobulin 1 (IgG1) -Fc-glycosylation profiling of anti-citrullinated peptide antibodies from human serum
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Immunoglobulin 1 (IgG1) -Fc-glycosylation profiling of anti-citrullinated peptide antibodies from human serum

机译:来自人血清的抗瓜氨酸化肽抗体的免疫球蛋白1(IgG1)-Fc-糖基化分析

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摘要

In several autoimmune disorders, including rheumatoid arthritis (RA), autoantibodies are thought to be the driving force of pathogenicity. Glycosylation of the Fc-part of human Igs is known to modulate biological activity. Hitherto, glycosylation of human IgG-Fc has been analyzed predominantly at the level of total serum IgG, revealing reduced galactosylation in RA. Given the pathogenic relevance of autoantibodies in RA, we wished, in the present study, to address the question whether distinct Fc-glycosylation features are observable at the level of antigen-specific IgG subpopulations. For this purpose, we have developed a method for the microscale purification and Fc-glycosylation analysis of anti-citrullinated peptide antibodies (ACPA). ACPA represent a group of autoantibodies that occur with unique specificity in RA patients. Their presence is associated with increased inflammatory disease activity and rapid joint destruction. Results indicate that ACPA of the IgG1 subclass vary considerably from total serum IgG1 with respect to Fc-galactosylation, with galactosylation being higher on ACPA than on serum IgG1 for some patients, while other patients show higher galactosylation on serum IgG1 than on ACPA. Using this method, studies can be performed on the biological and clinical relevance of ACPA glycosylation within RA patient cohorts.
机译:在包括风湿性关节炎(RA)在内的几种自身免疫性疾病中,自身抗体被认为是致病性的驱动力。已知人Igs的Fc部分的糖基化可调节生物活性。迄今为止,主要在总血清IgG水平上分析了人IgG-Fc的糖基化,揭示了RA中半乳糖基化的降低。考虑到RA中自身抗体的致病相关性,我们希望在本研究中解决在抗原特异性IgG亚群水平上是否可观察到不同的Fc-糖基化特征的问题。为此,我们开发了一种用于抗瓜氨酸化肽抗体(ACPA)的微量纯化和Fc-糖基化分析的方法。 ACPA代表一组在RA患者中具有独特特异性的自身抗体。它们的存在与炎性疾病活性增加和关节快速破坏有关。结果表明,相对于总血清IgG1,IgG1亚类的ACPA相对于Fc半乳糖基化有很大差异,某些患者在ACPA上的半乳糖基化高于血清IgG1,而其他患者在血清IgG1上的半乳糖基化高于ACPA。使用这种方法,可以对RA患者队列中ACPA糖基化的生物学和临床相关性进行研究。

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