首页> 外文期刊>Clinical rheumatology >Decreased IgG4 ACPA levels in responders and increased CD1c(+) classical dendritic cells in non-responders of patients with rheumatoid arthritis under therapy
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Decreased IgG4 ACPA levels in responders and increased CD1c(+) classical dendritic cells in non-responders of patients with rheumatoid arthritis under therapy

机译:治疗类风湿性关节炎患者的应答者 IgG4 ACPA 水平降低,无应答者 CD1c(+) 经典树突状细胞增加

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摘要

The treatment options for patients suffering from rheumatoid arthritis expanded over the last years. However, reliable biomarkers to guide therapy decisions are still warranted. Therefore, we here evaluated the value of antibodies against citrullinated peptide antigens (ACPA) IgG subclasses and peripheral blood antigen presenting cells as biomarkers to monitor and predict therapy response of patients with rheumatoid arthritis. Thirty-four ACPA-positive RA patients were enrolled and monitored for 3 months after therapy begin. ACPA IgG1 and IgG4 serum levels were quantified by ELISA. Phenotyping of the B cell, monocytic, and dendritic cell lineages was performed via flow cytometry. Three months after therapy begin, the responders showed a significant decrease in IgG4 ACPA levels, and this was independent of the individual treatment regimen. The non-responders showed a significant increase in CD1c(+) classical dendritic cells (cDC). Furthermore, the baseline disease activity score 28 and the baseline percentage of cDC allowed for some prediction of future therapy responses. We here suggest IgG4 ACPA levels as biomarkers to monitor therapy response in RA. The increase in CD1c(+) cDC among non-responders to therapy remains enigmatic and requires future elucidation of the underlying mechanisms.
机译:在过去几年中,类风湿性关节炎患者的治疗选择有所扩大。然而,仍然需要可靠的生物标志物来指导治疗决策。因此,我们在这里评估了针对瓜氨酸肽抗原 (ACPA) IgG 亚类和外周血抗原呈递细胞的抗体作为生物标志物监测和预测类风湿性关节炎患者治疗反应的价值。34 例 ACPA 阳性 RA 患者入组并在治疗开始后监测 3 个月。通过ELISA定量ACPA IgG1和IgG4血清水平。通过流式细胞术对 B 细胞、单核细胞和树突状细胞谱系进行表型分析。治疗开始三个月后,应答者显示 IgG4 ACPA 水平显着降低,这与个体治疗方案无关。无反应者显示CD1c(+)经典树突状细胞(cDC)显着增加。此外,基线疾病活动评分 28 和 cDC 的基线百分比允许对未来的治疗反应进行一些预测。我们在这里建议将 IgG4 ACPA 水平作为生物标志物来监测 RA 的治疗反应。对治疗无反应者中CD1c(+)cDC的增加仍然是个谜,需要未来阐明潜在的机制。

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