Identification of autoantibodies targeting citrullinated CLEC12A in rheumatoid arthritis patients

IF 4.7 Q2 IMMUNOLOGY

Journal of Translational Autoimmunity Pub Date : 2025-04-15 DOI:10.1016/j.jtauto.2025.100287

Lillian Barra , Sheri Saunders , Mathias Mangion , Guillaume Paré , Halim Maaroufi , Alain Garnier , Ewa Cairns , Maria J. Fernandes

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Abstract

Objective

Rheumatoid arthritis is an autoimmune disease characterized by anti-citrullinated protein antibodies (ACPA). The pathogenic and protective roles of ACPA of distinct specificities are emerging and remains poorly understood. Thus, it is crucial to define the range of ACPA specificities and determine their contribution to disease and their potential clinical relevance. Since extracellular citrullination occurs in RA, we investigated whether autoantibodies in RA patients bind a citrullinated form of the cell-surface receptor CLEC12A that is expressed on neutrophils, the most abundant leukocyte in inflamed joints.

Methods

We generated a FLAG-tagged, recombinant form of the extracellular portion of human CLEC12A. After purification, the tag was removed prior to citrullination by PAD2 that was confirmed by mass spectrometry. We developed an ELISA for citrullinated CLEC12A to screen for seropositivity in sera of 68 RA patients and 36 healthy controls. Potential associations between these autoantibodies and clinical variables were determined.

Results

In our cohort, 40 % of RA patients were positive for anti-citrullinated CLEC12A autoantibodies. Those seropositive patients were younger than RA patients that tested negative for these autoantibodies (p = 0.0058). Most patients had antibodies to multiple citrullinated and homocitrullinated antigens; 17 % of patients negative for other ACPA were positive for anti-citrullinated CLEC12A autoantibodies.

Conclusion

This is the first report of seropositivity towards citrullinated CLEC12A in RA patients. A validation cohort will confirm our findings and identify additional correlations between these autoantibodies and clinical parameters. Citrullination may be a mechanism through which CLEC12A's inhibitory function is altered to exacerbate inflammation in RA. Identifying citrullinated neoantigens advances our understanding of the diverse molecular mechanisms that contribute to RA pathogenesis.

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类风湿性关节炎患者瓜氨酸化cle12a自身抗体的鉴定

目的类风湿性关节炎是一种以抗瓜氨酸蛋白抗体（ACPA）为特征的自身免疫性疾病。具有不同特异性的 ACPA 的致病和保护作用正在逐渐显现，但人们对其了解甚少。因此，明确 ACPA 的特异性范围并确定它们对疾病的贡献及其潜在的临床意义至关重要。由于细胞外瓜氨酸化发生在RA中，我们研究了RA患者的自身抗体是否与细胞表面受体CLEC12A的瓜氨酸化形式结合，CLEC12A表达在中性粒细胞上，中性粒细胞是发炎关节中最多的白细胞。纯化后，在通过 PAD2 进行瓜氨酸化之前去除标签，并通过质谱法进行确认。我们开发了一种瓜氨酸化 CLEC12A 酶联免疫吸附试验（ELISA），以筛查 68 名 RA 患者和 36 名健康对照者血清中的血清阳性反应。结果在我们的队列中，40%的 RA 患者抗瓜氨酸化 CLEC12A 自身抗体呈阳性。这些血清阳性患者比这些自身抗体检测阴性的 RA 患者更年轻（p = 0.0058）。大多数患者体内存在多种瓜氨酸化和同型瓜氨酸化抗原抗体；17%其他ACPA检测阴性的患者体内抗瓜氨酸化CLEC12A自身抗体呈阳性。验证队列将证实我们的研究结果，并确定这些自身抗体与临床参数之间的其他相关性。瓜氨酸化可能是CLEC12A的抑制功能发生改变从而加剧RA炎症的一种机制。鉴定瓜氨酸化新抗原有助于我们了解导致RA发病机制的多种分子机制。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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