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Structural, antigenic and evolutionary analyses of immunoglobulins and T cell receptors.

机译:免疫球蛋白和T细胞受体的结构,抗原和进化分析。

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We have had the pleasure of collaborating with Allen Edmundson for the past 15 years on the structure, binding properties and evolution of immunoglobulins and T cell receptors. Among the most significant contributions of our joint efforts were: (1) the predictive use of structural features of immunoglobulin domains to model the three-dimensional structures of the immunoglobulin domains of human T-cell receptor alpha and beta chains as well as shark light chains and V(H) domains; (2) the finding that normal humans and other vertebrates express autoantibodies against combining site epitopes of their own T cell receptors; (3) the mapping of the peptide autoepitopes recognized in health, autoimmunity and retroviral infection; and (4) the determination that epitope recognition promiscuity is a characteristic property of the combining sites of IgM immunoglobulins ranging from those of sharks to those of humans. We briefly review the salient findings and status of these studies and indicate the future directions that we will pursue in their continuation.
机译:在过去的15年中,我们很高兴与艾伦·埃德蒙森(Allen Edmundson)在免疫球蛋白和T细胞受体的结构,结合特性和进化方面进行了合作。我们共同努力的最重要贡献之一是:(1)预测使用免疫球蛋白结构域的结构特征来模拟人T细胞受体α和β链以及鲨鱼轻链的免疫球蛋白域的三维结构和V(H)域; (2)发现正常人和其他脊椎动物表达针对自身T细胞受体结合位点表位的自身抗体; (3)在健康,自身免疫和逆转录病毒感染中公认的肽自身表位的定位; (4)确定表位识别混杂是IgM免疫球蛋白结合位点(从鲨鱼到人的范围)的特征。我们简要回顾了这些研究的主要发现和现状,并指出了我们将继续进行的未来发展方向。

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