首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >A method for producing monoclonal antibodies to human T-cell-receptor beta-chain variable regions.
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A method for producing monoclonal antibodies to human T-cell-receptor beta-chain variable regions.

机译:一种产生针对人T细胞受体β链可变区的单克隆抗体的方法。

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摘要

Study of the T-cell repertoire in humans has been hampered by the lack of monoclonal antibodies (mAbs) to the T-cell receptor (TCR) variable region (V) gene products. We describe a method for producing mAbs to the human TCR beta-chain V (V beta) gene products in which mice were immunized with a rat basophil cell line (RBL-2H3) transfected with the extracellular domain of the TCR heterodimer fused to the lambda chain of CD3. These cells acted as excellent immunogens for raising anti-TCR mAb and also formed the basis of a rapid screening assay. We generated mAbs against V beta protein of the TCR, showed that these mAbs stained approximately 1% of peripheral blood T cells, and further showed that the mAbs could stimulate proliferation of these T cells. We then characterized the mAbs by amplifying TCR cDNA derived from mAb-stimulated cells and sequencing the beta chain. All clones sequenced used the V beta 7.1 chain, proving conclusively that the mAbs generated were specific for V beta 7.1 subfamily. This method generates mAbs to human TCR V beta proteins efficiently and might allow production of a complete panel of mAbs directed against human TCR V beta proteins.
机译:由于缺乏针对T细胞受体(TCR)可变区(V)基因产物的单克隆抗体(mAb),阻碍了人类T细胞库的研究。我们描述了一种生产人TCRβ链V(V beta)基因产物的单克隆抗体的方法,其中小鼠用大鼠嗜碱性粒细胞系(RBL-2H3)免疫,转染了lambda的TCR异源二聚体的胞外域转染了大鼠嗜碱性粒细胞系CD3链。这些细胞充当了提高抗TCR mAb的极佳免疫原,并且也构成了快速筛选测定的基础。我们生成了针对TCR Vβ蛋白的mAb,表明这些mAb染色了大约1%的外周血T细胞,并进一步表明mAb可以刺激这些T细胞的增殖。然后,我们通过扩增源自mAb刺激的细胞的TCR cDNA并对β链进行测序来表征mAb。所有测序的克隆均使用V beta 7.1链,最终证明产生的mAb对V beta 7.1亚家族具有特异性。该方法有效地产生针对人TCR Vβ蛋白的mAb,并且可能允许产生针对人TCR Vβ蛋白的完整mAb面板。

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