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天然配对的人 T 细胞受体库的永生化和功能筛选。

Immortalization and functional screening of natively paired human T cell receptor repertoires.

机构信息

Department of Pharmaceutical Chemistry, The University of Kansas, Lawrence, KS 66044, USA.

Vaccine Research Center, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Protein Eng Des Sel. 2022 Feb 17;35. doi: 10.1093/protein/gzab034.

Abstract

Functional analyses of the T cell receptor (TCR) landscape can reveal critical information about protection from disease and molecular responses to vaccines. However, it has proven difficult to combine advanced next-generation sequencing technologies with methods to decode the peptide-major histocompatibility complex (pMHC) specificity of individual TCRs. We developed a new high-throughput approach to enable repertoire-scale functional evaluations of natively paired TCRs. In particular, we leveraged the immortalized nature of physically linked TCRα:β amplicon libraries to analyze binding against multiple recombinant pMHCs on a repertoire scale, and to exemplify the utility of this approach, we also performed affinity-based functional mapping in conjunction with quantitative next-generation sequencing to track antigen-specific TCRs. These data successfully validated a new immortalization and screening platform to facilitate detailed molecular analyses of disease-relevant antigen interactions with human TCRs.

摘要

功能分析 T 细胞受体 (TCR) 景观可以揭示关于疾病保护和疫苗分子反应的关键信息。然而,将先进的下一代测序技术与解码个体 TCR 的肽-主要组织相容性复合体 (pMHC) 特异性的方法结合起来一直具有挑战性。我们开发了一种新的高通量方法,能够对天然配对的 TCR 进行功能评估。具体来说,我们利用物理连接的 TCRα:β 扩增文库的永生性质,在文库范围内分析针对多种重组 pMHC 的结合,并且为了说明这种方法的实用性,我们还进行了基于亲和力的功能映射,结合定量下一代测序来跟踪抗原特异性 TCR。这些数据成功验证了一种新的永生和筛选平台,以促进对人类 TCR 与疾病相关抗原相互作用的详细分子分析。

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