Specific Features of Juvenile Idiopathic Arthritis Patients' Chemokine Profile: The Data of Case-Control Study Analysis.

IF 1.2 Q4 RHEUMATOLOGY Current rheumatology reviews Pub Date : 2024-09-05 DOI:10.2174/0115733971308074240813060452
Arseniy V Rybakov, Karina A Yureva, Vitaliy V Khizha, Darya I Kozlova, Lybov S Sorokina, Vyacheslav I Zorin, Aleksei N Kozhevnikov, Mikhail M Kostik
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Abstract

Background: Juvenile idiopathic arthritis pathogenesis involves a large number of different immune system cells, which are both sources and targets of chemokines, that affect not only their migration but also survival, proliferation, differentiation, production of all cytokine types, degranulation, and also directly stimulating or suppressing angiogenesis. Studyingthe contribution of chemokines to this disease pathogenesis will make it possible to identify new sensitive and specific markers for its diagnosis and subsequent dynamic monitoring of treatment effectiveness. The study aimed to identify a list of the most informative diagnostic markers from a wide range of juvenile idiopathic arthritis patients' blood plasma chemokines.

Methods: The case-control study included 40 diagnosed pathology patients and 20 healthy agematched children. The content of MCP-1/CCL2, MCP-3/CCL7, MIG/CXCL9, MIP-1α/CCL3, MIP-1β/CCL4, RANTES/CCL5, IFN-γ, IP-10/CXCL10, and MDC/CCL22 were measured by enzyme- linked immunosorbent assay in blood plasma of each person.

Results: The following chemokines were included in the list of the most promising diagnostic markers: MCP-1, MIP-1α, MIG, RANTES, and IFN-γ. Their blood plasma content in patients with a diagnosed pathology was from 3 to 60 times (MIG) higher than in the conditionally healthy group. Their sensitivity and specificity exceeded 90%.

Conclusion: An increase in their content leads to active monocytes/macrophages migration to the site of inflammation, where they suppress effector T-cell activity by binding suppressor exosomes and activate B-cells by autoantigens presentation received due to joint tissue destruction. This allows us to speak about the predominance of the Th1-mediated immune response during the development of studied disease chronic inflammation.

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幼年特发性关节炎患者化学因子谱的具体特征:病例对照研究分析数据
背景:趋化因子不仅影响细胞的迁移,还影响细胞的存活、增殖、分化、所有细胞因子类型的产生、脱颗粒以及直接刺激或抑制血管生成。研究趋化因子对这种疾病发病机制的作用,将有可能确定新的敏感和特异性标记物,用于诊断和随后对治疗效果进行动态监测。该研究旨在从大量幼年特发性关节炎患者的血浆趋化因子中找出最有参考价值的诊断标记物:病例对照研究包括40名确诊病理的患者和20名年龄匹配的健康儿童。方法:该病例对照研究纳入了 40 名确诊病理患者和 20 名年龄相仿的健康儿童,通过酶联免疫吸附试验测定了每人血浆中 MCP-1/CCL2、MCP-3/CCL7、MIG/CXCL9、MIP-1α/CCL3、MIP-1β/CCL4、RANTES/CCL5、IFN-γ、IP-10/CXCL10 和 MDC/CCL22 的含量:结果:下列趋化因子被列入最有希望的诊断标记物名单:MCP-1、MIP-1α、MIG、RANTES 和 IFN-γ。在确诊病变的患者血浆中,这些指标的含量比条件健康组高 3 到 60 倍(MIG)。其敏感性和特异性均超过 90%:其含量的增加会导致活跃的单核细胞/巨噬细胞迁移到炎症部位,它们通过结合抑制性外泌体抑制效应 T 细胞的活性,并通过关节组织破坏导致的自身抗原呈递激活 B 细胞。因此,我们可以说,在所研究疾病的慢性炎症发展过程中,Th1 介导的免疫反应占主导地位。
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来源期刊
CiteScore
2.30
自引率
0.00%
发文量
82
期刊介绍: Current Rheumatology Reviews publishes frontier reviews on all the latest advances on rheumatology and its related areas e.g. pharmacology, pathogenesis, epidemiology, clinical care, and therapy. The journal"s aim is to publish the highest quality review articles dedicated to clinical research in the field. The journal is essential reading for all researchers and clinicians in rheumatology.
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