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首页> 外文期刊>Rheumatology >Ankylosing spondylitis patients display altered dendritic cell and T cell populations that implicate pathogenic roles for the IL-23 cytokine axis and intestinal inflammation
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Ankylosing spondylitis patients display altered dendritic cell and T cell populations that implicate pathogenic roles for the IL-23 cytokine axis and intestinal inflammation

机译:强直性脊柱炎患者的树突状细胞和T细胞数量发生变化,这暗示了IL-23细胞因子轴和肠道炎症的致病作用

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摘要

Objective. AS is a systemic inflammatory disease of the SpA family. Polymorphisms at loci including HLA-B27, IL-23R and ERAP-1 directly implicate immune mechanisms in AS pathogenesis. Previously, in an SpA model, we identified HLA-B27-mediated effects on dendritic cells that promoted disease-associated Th17 cells. Here we extend these studies to AS patients using deep immunophenotyping of candidate pathogenic cell populations. The aim of our study was to functionally characterize the immune populations mediating AS pathology.
机译:目的。 AS是SpA家族的全身性炎性疾病。 HLA-B27,IL-23R和ERAP-1等基因座的多态性直接暗示了AS发病机制中的免疫机制。以前,在SpA模型中,我们鉴定了HLA-B27介导的树突状细胞对疾病相关Th17细胞的促进作用。在这里,我们使用候选病原细胞群体的深层免疫表型将这些研究扩展到AS患者。我们研究的目的是在功能上表征介导AS病理的免疫种群。

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