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A novel strategy to identify autoantigens by proteomic analysis of plasma IgG-bound proteins

机译:血浆IgG结合蛋白蛋白质组学分析鉴定自身抗原的一种新策略

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Autoimmune mechanisms have been hypothesized to underlie a number of human disorders in which both disease pathogenesis and diagnostic biomarkers remain poorly understood. This is partly due to a lack of efficient techniques for identification of plasma autoantibodies associated with specific pathophysiological conditions. We have developed a novel proteomic methodology to comprehensively identify plasma IgG-bound proteins using liquid chromatography tandem mass spectrometry (LC-MS/MS) after denaturing enriched plasma IgG to solubilize and release low molecular weight proteins. In total, we identified 44 proteins using this method that were undetectable in unprocessed plasma, 21 of which were not identified in the Human Plasma Proteome Draft of 2017. Comparison of plasma IgG-bound proteins between healthy subjects and patients with isolated adrenocorticotropic hormone deficiency, a rare endocrine disorder speculated to involve autoimmune mechanisms, revealed several distinct IgG-bound proteins specifically detected in patient plasma but not in healthy subjects. Our results suggest that solubilization of low molecular weight proteins bound to enriched plasma IgG and subsequent proteomic analysis by LC-MS/MS could provide a promising strategy for identification of autoantigens in human peripheral blood.
机译:自身免疫机制已被假设为使得疾病发病机制和诊断生物标志物仍然明白的许多人类疾病。这部分是由于缺乏有效的技术,用于鉴定与特定病理生理病症相关的血浆自身抗体。我们开发了一种新颖的蛋白质组学方法,以在变性富集的等离子体IgG后综合鉴定液相色谱串联质谱(LC-MS / MS)以溶解和释放低分子量蛋白质之后的液相色谱串联质谱(LC-MS / MS)。总共使用该方法确定了44种蛋白质,其在未加工的血浆中未检测到,其中21例未在2017年人血浆蛋白质组草稿中鉴定。健康受试者和患者患者患者血糖肾上腺激素缺乏症之间的血浆IgG结合蛋白的比较,推测的稀有内分泌疾病涉及自身免疫机制,揭示了在患者血浆中特异性检测到的几种不同的IgG结合的蛋白质,但不在健康受试者中。我们的研究结果表明,LC-MS / MS中结合富集的血浆IgG和随后的蛋白质组学分析的低分子量蛋白质的溶解可以提供有希望的鉴定人周围血液中自身抗原的策略。

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