首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >The epitopes targeted by the rheumatoid arthritis-associated antifilaggrin autoantibodies are posttranslationally generated on various sites of (pro)filaggrin by deimination of arginine residues.
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The epitopes targeted by the rheumatoid arthritis-associated antifilaggrin autoantibodies are posttranslationally generated on various sites of (pro)filaggrin by deimination of arginine residues.

机译:由类风湿关节炎相关的抗丝聚素自身抗体靶向的表位是通过精氨酸残基的脱除在翻译后在(聚)丝聚素的多个位点上产生的。

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摘要

Antifilaggrin autoantibodies (AFA) are a population of IgG autoantibodies associated to rheumatoid arthritis (RA), which includes the so-called "antikeratin" Abs and antiperinuclear factor. AFA are the most specific serological markers of RA. We previously showed that they recognize human epidermal filaggrin and other profilaggrin-related proteins of various epithelial tissues. Here, we report further characterization of the protein Ags and epitopes targeted by AFA. All the Ags that exhibit numerous neutral/ acidic isoelectric variants were immunochemically demonstrated to be deiminated proteins. In vitro deimination of a recombinant human filaggrin by a peptidylarginine deiminase generated AFA epitopes on the protein. Moreover, two of three filaggrin-derived synthetic peptides with a citrulline in the central position were specifically and widely recognized by AFA affinity-purified from a series of RA sera. These results indicate that citrulline residues are constitutive of the AFA epitopes, but only in the context of specific amino acid sequences of filaggrin. In competition experiments, the two peptides abolished the AFA reactivity of RA sera, showing that they present major AFA epitopes. These data should help in the identification of a putative deiminated AFA-inducing or cross-reactive articular autoantigen and provide new insights into the pathogenesis of RA. They could also open the way toward specific immunosuppressive and/or preventive therapy of RA.
机译:抗丝蛋白自身抗体(AFA)是与类风湿关节炎(RA)相关的IgG自身抗体群体,其中包括所谓的“抗角蛋白”抗体和抗核素因子。 AFA是RA最具体的血清学指标。我们以前的研究表明,它们可以识别人类上皮中的丝聚蛋白和各种上皮组织的其他与丝聚蛋白相关的蛋白质。在这里,我们报道了AFA靶向的蛋白质Ags和表位的进一步表征。免疫化学证明所有表现出许多中性/酸性等电变异的Ags都是脱蛋白质。肽基精氨酸脱亚氨酶在体外对重组人丝聚蛋白进行脱氨反应,在蛋白质上产生AFA表位。此外,通过一系列RA血清亲和纯化的AFA特异性地广泛识别了中心位置具有瓜氨酸的三种丝氨酸衍生合成肽中的两种。这些结果表明瓜氨酸残基是AFA表位的组成,但是仅在丝聚蛋白的特定氨基酸序列的背景下。在竞争实验中,这两种肽消除了RA血清的AFA反应性,表明它们呈现出主要的AFA表位。这些数据应有助于鉴定推定的AFA诱导或交叉反应性关节自身抗原,并为RA的发病机理提供新的见解。他们还可以为RA的特异性免疫抑制和/或预防疗法开辟道路。

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