首页> 外文期刊>Annals of the Rheumatic Diseases: A Journal of Clinical Rheumatology and Connective Tissue Research >Distribution and clinical significance of blood dendritic cells in children with juvenile idiopathic arthritis.
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Distribution and clinical significance of blood dendritic cells in children with juvenile idiopathic arthritis.

机译:幼年特发性关节炎儿童血液树突状细胞的分布及其临床意义。

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BACKGROUND: A role for dendritic cells (DC) in the development of adult rheumatoid arthritis has been suggested. To date, this problem has been poorly explored in juvenile idiopathic arthritis (JIA). OBJECTIVE: To analyse distribution and maturation status of blood DC (BDC) in JIA. METHODS: Absolute BDC counts were assessed by the "single platform" method in peripheral blood (PB) of 47 untreated children with JIA and 32 healthy controls. Moreover, BDC were investigated in JIA synovial fluid (SF). When the panel of monoclonal antibodies against BDC antigens (BDCA) was used, three BDC subpopulations were determined: myeloid type 1 (mDC1; BDCA-1+/HLA-DR+/CD19-), myeloid type 2 (mDC2; BDCA-3+/HLA-DR+/CD14-) and plasmacytoid (pDC; BDCA-2+/HLA-DR+/CD123+). RESULTS: A considerable deficiency of all subtypes of BDC was found in the PB of children with JIA. BDC counts in JIA SF were significantly higher than in PB both from children with JIA (p<0.001) and healthy children (p<0.001). SF BDC, especially mDC1 and mDC2 subtypes, had significantly higher expression of maturation markers (CD40, CD80, CD86 or CD83 antigens) than those from PB. A smaller number of PB BDC at diagnosis correlated significantly with poor response to treatment. CONCLUSIONS: A deficiency of BDC in PB is accompanied by enrichment of SF with those cells. Probably, circulating BDC migrate to joints where they undergo maturation and help to mediate and maintain the local immune response. Interestingly, the level of PD BDC deficiency seems to influence the outcome in children with JIA.
机译:背景:已经提出树突状细胞(DC)在成人类风湿性关节炎发展中的作用。迄今为止,在青少年特发性关节炎(JIA)中尚未很好地探讨此问题。目的:分析JIA中血液DC(BDC)的分布和成熟状况。方法:采用“单一平台”方法评估47名未经治疗的JIA儿童和32名健康对照者的外周血(PB)的绝对BDC计数。此外,在JIA滑液(SF)中研究了BDC。当使用一组针对BDC抗原的单克隆抗体(BDCA)时,确定了三个BDC亚群:髓样1型(mDC1; BDCA-1 + / HLA-DR + / CD19-),髓样2型(mDC2; BDCA-3 + / HLA-DR + / CD14-)和浆细胞样(pDC; BDCA-2 + / HLA-DR + / CD123 +)。结果:在JIA患儿的PB中发现了BDC所有亚型的显着缺乏。无论是JIA儿童(p <0.001)还是健康儿童(p <0.001),JIA SF的BDC计数均显着高于PB。 SF BDC,尤其是mDC1和mDC2亚型,其成熟标记(CD40,CD80,CD86或CD83抗原)的表达明显高于PB。诊断时较少的PB BDC与治疗反应差相关。结论:PB中BDC缺乏伴随着那些细胞富集SF。循环中的BDC可能会迁移到关节处,并在那里进行成熟并有助于介导和维持局部免疫应答。有趣的是,PD BDC缺乏水平似乎会影响JIA儿童的预后。

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