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首页> 外文期刊>International immunology. >Divergence in the degree of clonal expansions in inflammatory T cell subpopulations mirrors HLA-associated risk alleles in genetically and clinically distinct subtypes of childhood arthritis.
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Divergence in the degree of clonal expansions in inflammatory T cell subpopulations mirrors HLA-associated risk alleles in genetically and clinically distinct subtypes of childhood arthritis.

机译:炎性T细胞亚群克隆扩增程度的差异反映了儿童关节炎的遗传和临床不同亚型中与HLA相关的风险等位基因。

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摘要

Clinically distinct forms of childhood arthritis are associated with different risk alleles of polymorphic loci within the MHC, which code for the antigen-presenting class I or class II molecules. We have compared the TCR diversity of synovial T cells from children with enthesitis-related (HLA-B27(+)) arthritis and oligoarticular arthritis (with class II MHC risk allele associations) in parallel with peripheral blood T cells from each child, using a high-resolution heteroduplex TCR analysis. We demonstrate that multiple clonal T cell expansions are present and persistent within the joint in both groups, but that there is disease-specific divergence in the dominant T cell subset containing these expansions. Thus, the largest clonotypes within the inflamed joints of children with class II-associated arthritis are within the CD4(+) synovial T cell population, while the dominant clones from children with enthesitis-related arthritis (associated with a class I allele) are within the CD8(+) synovial T cell population. These data provide powerful data to support the concept that recognition of MHC-peptide complexes by T cells plays a role in the pathogenesis of juvenile arthritis.
机译:儿童关节炎的临床上不同形式与MHC中多态性基因座的不同风险等位基因相关,后者编码抗原呈递I类或II类分子。我们比较了与每个儿童外周血T细胞平行的,患有脑炎相关性(HLA-B27(+))关节炎和少关节关节炎(具有II类MHC风险等位基因关联)的儿童的滑膜T细胞的TCR多样性。高分辨率异源双链TCR分析。我们证明了在两组中关节内均存在并持续存在多个克隆性T细胞扩增,但是在包含这些扩增的显性T细胞亚群中存在疾病特异性的分化。因此,与II类关节炎相关的儿童发炎关节内最大的克隆型位于CD4(+)滑膜T细胞群体中,而与患有肠炎相关关节炎的儿童(与I类等位基因相关)的显性克隆位于CD8(+)滑膜T细胞群体。这些数据提供了有力的数据,以支持T细胞识别MHC肽复合物在青少年关节炎的发病机理中起作用的概念。

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