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首页> 外文期刊>Arthritis research & therapy. >Antibody responses to de novo identified citrullinated fibrinogen peptides in rheumatoid arthritis and visualization of the corresponding B cells
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Antibody responses to de novo identified citrullinated fibrinogen peptides in rheumatoid arthritis and visualization of the corresponding B cells

机译:类风湿关节炎中从头鉴定的瓜氨酸化纤维蛋白原肽的抗体应答和相应B细胞的可视化

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摘要

Background Antibodies against citrullinated proteins (ACPA) are common in patients with rheumatoid arthritis (RA). ACPA can appear before disease onset and target many self-antigens. Citrullinated fibrin/fibrinogen represents a classical ACPA target antigen, and mass spectrometry of RA synovial fluid reveals elevated citrullinated (cit) fibrinogen (Fib) peptides compared to non-RA controls. We investigated the extent to which these less-studied peptides represent autoantibody targets and sought to visualize the corresponding cit-Fib-reactive B cells in RA patients. Methods An in-house ELISA was established against four cit-Fib α-subunit peptides (cit-Fib α-35; cit-Fib α-216,218; cit-Fib α-263,271 and cit-Fib α-425,426) and serum from patients with established RA ( n =?347) and disease controls with psoriatic arthritis (PsA) or ankylosing spondylitis (AS) ( n =?236) were analyzed. RA patients were genotyped for HLA-DR alleles, PTPN22 R620W and screened for anti-CCP2 and cit-Fib protein antibodies. The cit-Fib peptides were also used to assemble antigen tetramers to identify cit-Fib-reactive B cells in peripheral blood by flow cytometry. Results The frequencies of autoantibodies against different cit-Fib epitopes in RA patients compared to PsA/AS patients were: cit-Fib α-35 (RA 20%, vs PsA/AS 1%); cit-Fib α-216,218 (13% vs 0.5%); cit-Fib α-263,271 (21% vs 0.5%) and cit-Fib α-425,426 (17% vs 1%). The presence of autoantibodies against these peptides was associated with presence of anti-CCP2 and anti-cit-Fib protein antibodies. No association was found between HLA-DR shared epitope and antibodies to the different cit-Fib peptides. However, association was observed between the PTPN22 risk allele and positivity to cit-Fib α-35 and cit-Fib α-263,271. B cells carrying surface Ig reactive to these cit-Fib peptides were found in RA peripheral blood and these tend to be more common in PTPN22 risk allele carriers. Conclusions Our data show that several cit-Fib peptides are targeted by autoantibodies in RA, but not in PsA/AS, implicating that these are not due to arthritis but more specific for RA etiology. The RA-associated anti-cit protein response is broad with many parallel immune responses. The association between cit-Fib autoantibodies and the PTPN22 R620W risk allele supports the hypothesis of altered B cell regulation, such as autoreactive B cells evading tolerance checkpoints.
机译:背景技术类风湿性关节炎(RA)患者常见抗瓜氨酸化蛋白(ACPA)的抗体。 ACPA可以在疾病发作之前出现,并靶向许多自身抗原。瓜氨酸化纤维蛋白/纤维蛋白原代表经典的ACPA靶抗原,RA滑液的质谱分析显示,与非RA对照相比,瓜氨酸化(cit)纤维蛋白原(Fib)肽含量升高。我们调查了这些研究较少的肽代表自身抗体靶标的程度,并试图可视化RA患者中相应的cit-Fib反应性B细胞。方法建立内部ELISA,对患者的四种cit-Fibα-亚基肽(cit-Fibα-35; cit-Fibα-216,218; cit-Fibα-263,271和cit-Fibα-425,426)和血清进行检测已确定RA(n = 347)和银屑病关节炎(PsA)或强直性脊柱炎(AS)(n = 236)的疾病对照。对RA患者进行HLA-DR等位基因,PTPN22 R620W基因分型,并筛选抗CCP2和cit-Fib蛋白抗体。 cit-Fib肽还用于组装抗原四聚体,以通过流式细胞术鉴定外周血中的cit-Fib反应性B细胞。结果与PsA / AS患者相比,RA患者针对不同cit-Fib表位的自身抗体的频率为:cit-Fibα-35(RA为20%,PsA / AS为1%); cit-Fibα-216,218(13%比0.5%); cit-Fibα-263,271(21%vs 0.5%)和cit-Fibα-425,426(17%vs 1%)。针对这些肽的自身抗体的存在与抗CCP2和抗cit-Fib蛋白抗体的存在相关。在HLA-DR共享表位和针对不同cit-Fib肽的抗体之间未发现关联。但是,在PTPN22风险等位基因与对cit-Fibα-35和cit-Fibα-263,271的阳性之间观察到关联。在RA外周血中发现了带有对这些cit-Fib肽具有反应性的表面Ig的B细胞,这些B细胞在PTPN22高风险等位基因携带者中更常见。结论我们的数据表明RA中的自身抗体靶向了几种cit-Fib肽,但PsA / AS中没有这种抗体,这暗示它们不是由于关节炎引起的,而是对RA病因更具特异性。 RA相关的抗cit蛋白应答广泛,具有许多平行的免疫应答。 cit-Fib自身抗体与PTPN22 R620W风险等位基因之间的关联支持B细胞调节改变的假设,例如自身反应性B细胞逃避耐受性检查点。

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