首页> 美国卫生研究院文献>The Journal of Clinical Investigation >Disease-associated human histocompatibility leukocyte antigen determinants in patients with seropositive rheumatoid arthritis. Functional role in antigen-specific and allogeneic T cell recognition.
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Disease-associated human histocompatibility leukocyte antigen determinants in patients with seropositive rheumatoid arthritis. Functional role in antigen-specific and allogeneic T cell recognition.

机译:血清反应阳性类风湿关节炎患者中与疾病相关的人类组织相容性白细胞抗原决定簇。在抗原特异性和同种异体T细胞识别中的功能作用。

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摘要

The susceptibility to develop seropositive rheumatoid arthritis (RA) has been linked to specific genomic polymorphisms within the HLA complex. Two different haplotypes have been associated with the disease, HLA-DR1 and HLA-DR4. To investigate the link between such phenotypic disease associations and potential immune mechanisms we used alloreactive and antigen-specific human T cell clones. Here we describe a panel of alloreactive T cell clones directed to polymorphic determinants encoded by the third hypervariable region (hvr) of the HLA-DR beta 1-chain. T cell determinants defined by these clones are shared among HLA-DR1, HLA-Dw4, HLA-Dw13, HLA-Dw14, and HLA-Dw15, and are frequent in a population of RA patients. To study the role of such disease-associated epitopes in antigen-restricted T cell recognition we generated T cell clones from RA patients specific for mycobacterial antigens, Epstein-Barr virus antigens, and tetanus toxoid. In all three antigenic systems T cell clones were restricted to either HLA-DR1 or HLA-DR4. These data suggest that the polymorphisms within the first and second hvr of the HLA-DR beta 1-chain that are distinct in HLA-DR1 and HLA-DR4 and not associated with the disease are crucially involved in the recognition of antigens. Polymorphic determinants encoded by the third hvr are shared among disease-associated haplotypes and may function to mediate the interaction of alloreactive T cell receptor molecules with the HLA complex.
机译:发生血清反应阳性类风湿性关节炎(RA)的敏感性与HLA复合体内的特定基因组多态性有关。该疾病与两种不同的单倍型相关,即HLA-DR1和HLA-DR4。为了研究这种表型疾病关联和潜在的免疫机制之间的联系,我们使用了同种反应性和抗原特异性的人类T细胞克隆。在这里,我们描述了一组针对由HLA-DR beta 1链的第三高变区(hvr)编码的多态决定簇的同种反应性T细胞克隆。这些克隆定义的T细胞决定簇在HLA-DR1,HLA-Dw4,HLA-Dw13,HLA-Dw14和HLA-Dw15之间共享,并且在RA患者人群中很常见。为了研究这种与疾病相关的表位在抗原限制的T细胞识别中的作用,我们从RA患者中产生了分枝杆菌抗原,爱泼斯坦-巴尔病毒抗原和破伤风类毒素特异的T细胞克隆。在所有三个抗原系统中,T细胞克隆都限于HLA-DR1或HLA-DR4。这些数据表明在HLA-DR1和HLA-DR4中不同且与疾病无关的HLA-DR beta 1链的第一和第二条hvr内的多态性与抗原的识别至关重要。由第三种hvr编码的多态性决定簇在与疾病相关的单倍型之间共享,并可能起介导同种反应性T细胞受体分子与HLA复合物相互作用的作用。

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