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在TCR转基因小鼠中具有完全功能的HLA B27限制性CD4+以及CD8+ T细胞应答。

Fully functional HLA B27-restricted CD4+ as well as CD8+ T cell responses in TCR transgenic mice.

作者信息

Roddis Matthew, Carter Robert W, Sun Mei-Yi, Weissensteiner Thomas, McMichael Andrew J, Bowness Paul, Bodmer Helen C

机构信息

Edward Jenner Institute for Vaccine Research, Compton, Nr. Newbury, Berkshire RG 20 7NN, United Kingdom.

出版信息

J Immunol. 2004 Jan 1;172(1):155-61. doi: 10.4049/jimmunol.172.1.155.

Abstract

The strong association of HLA B27 with spondyloarthropathies contrasts strikingly with most autoimmune diseases, which are HLA class II associated and thought to be mediated by CD4+ T lymphocytes. By introducing a human-derived HLA B27-restricted TCR into HLA B27 transgenic mice, we have obtained a functional TCR transgenic model, GRb, dependent on HLA B27 for response. Surprisingly, HLA B27 supported CD4+ as well as CD8+ T cell responses in vivo and in vitro. Further, HLA B27-restricted CD4+ T cells were capable of differentiation into a range of Th1 and Th2 T cell subsets with normal patterns of cytokine expression. The transgenic T cells were also able to enhance clearance of recombinant vaccinia virus containing influenza nucleoprotein in vivo. This is the first description of a human HLA class I-restricted TCR transgenic line. The existence of CD4+ MHC class I-restricted T cells has significant implications for immune regulation in autoimmunity and, in particular, in HLA B27-associated arthritis. We believe that this model provides a novel system for the study of unusual T cell behavior in vivo.

摘要

HLA B27与脊柱关节病的紧密关联与大多数自身免疫性疾病形成鲜明对比,后者与HLA II类相关,且被认为是由CD4+ T淋巴细胞介导的。通过将人源HLA B27限制性TCR引入HLA B27转基因小鼠,我们获得了一个功能性TCR转基因模型GRb,其反应依赖于HLA B27。令人惊讶的是,HLA B27在体内和体外均支持CD4+以及CD8+ T细胞反应。此外,HLA B27限制性CD4+ T细胞能够分化为一系列具有正常细胞因子表达模式的Th1和Th2 T细胞亚群。转基因T细胞在体内也能够增强对含有流感核蛋白的重组痘苗病毒的清除。这是对人HLA I类限制性TCR转基因系的首次描述。CD4+ MHC I类限制性T细胞的存在对自身免疫中的免疫调节具有重要意义,尤其是在HLA B27相关关节炎中。我们认为该模型为研究体内异常T细胞行为提供了一个新系统。

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