Immortalization and Functional Screening of Natively Paired Human T Cell Receptor Repertoires

Author:

Fahad Ahmed S.ORCID,Chung Cheng Yu,Lopez Acevedo Sheila N.,Boyle Nicoleen,Madan Bharat,Gutiérrez-González Matias F.,Matus-Nicodemos Rodrigo,Laflin Amy D.,Ladi Rukmini R.,Zhou John,Wolfe Jacy,Llewellyn-Lacey Sian,Douek Daniel C.,Balfour Henry H.,Price David A.,DeKosky Brandon J.ORCID

Abstract

AbstractFunctional 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. Here 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. 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 human TCRs against diverse antigen targets associated with health, vaccination, or disease.

Publisher

Cold Spring Harbor Laboratory

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