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Secretion of a soluble, chimeric gamma delta T-cell receptor-immunoglobulin heterodimer.

机译:可溶性嵌合γ-T细胞受体-免疫球蛋白异二聚体的分泌。

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摘要

Soluble derivatives of T-cell antigen receptors (TCRs) should prove invaluable for studying the interaction of these receptors with antigens and major histocompatibility complex molecules, for structural studies, and for the identification of unknown ligands. We have engineered chimeric proteins, containing the extracellular domains of the mouse V gamma 1.1-C gamma 4 and V delta 6.2-C delta (V, variable; C, constant) TCR chains fused to the hinge region, CH2 (H, heavy), and CH3 domains of human IgG1 heavy chain, and expressed them by transient transfection in COS cells. We show here that TCR gamma-IgH and TCR delta-IgH chimeric chains are produced intracellularly in significant amounts, that the two chains can assemble correctly to form disulfide-linked, glycosylated heterodimers, and that a selective mechanism allows secretion of correctly paired receptor chains into the medium. Identity of the chimeric secreted TCR gamma delta-IgH heterodimer was confirmed by immunoblot analysis using V gamma 1-specific anti-peptide antiserum and immunoprecipitation analysis using the monoclonal antibody UC7, which is shown to be specific for the TCR delta chain. In addition, the soluble TCR gamma delta-IgH heterodimer can be immunoprecipitated with the anti-clonotypic monoclonal antibody F10/56, which suggests that the fusion protein likely has a structural conformation similar to that of the native TCR. The COS cell expression system may prove useful for the production of additional TCR-IgH fusion proteins.
机译:T细胞抗原受体(TCR)的可溶性衍生物对于研究这些受体与抗原和主要的组织相容性复合物分子的相互作用,进行结构研究以及鉴定未知的配体应被证明具有无价的价值。我们设计了嵌合蛋白,其中包含与融合到铰链区CH2(H,重)的小鼠Vγ1.1-Cγ4和Vδ6.2-Cδ(V,可变; C,恒定)TCR链的胞外域。和人IgG1重链的CH3域,并通过在COS细胞中瞬时转染来表达它们。我们在这里显示,TCRγ-IgH和TCRδ-IgH嵌合链在细胞内大量产生,两条链可以正确组装以形成二硫键连接的糖基化异二聚体,并且选择性机制可以分泌正确配对的受体链进入媒体。嵌合分泌的TCRγ-IgH异二聚体的身份通过使用Vγ1特异性抗肽抗血清的免疫印迹分析和使用单克隆抗体UC7的免疫沉淀分析得到证实,该单克隆抗体被证明对TCRδ链具有特异性。此外,可用抗克隆型单克隆抗体F10 / 56免疫沉淀可溶性TCRγ-IgH异二聚体,这表明融合蛋白可能具有与天然TCR相似的结构构象。 COS细胞表达系统可能被证明可用于生产其他TCR-IgH融合蛋白。

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