Author:
Fahad Ahmed S.,Chung Cheng Yu,López Acevedo Sheila N.,Boyle Nicoleen,Madan Bharat,Gutiérrez-González Matías F.,Matus-Nicodemos Rodrigo,Laflin Amy D.,Ladi Rukmini R.,Zhou John,Wolfe Jacy,Llewellyn-Lacey Sian,Koup Richard A.,Douek Daniel C.,Balfour Henry H.,Price David A.,DeKosky Brandon J.
Abstract
AbstractAdoptive immune therapies based on the transfer of antigen-specific T cells have been used successfully to treat various cancers and viral infections, but improved techniques are needed to identify optimally protective human T cell receptors (TCRs). Here we present a high-throughput approach to the identification of natively paired human TCRα and TCRβ (TCRα:β) genes encoding heterodimeric TCRs that recognize specific peptide antigens bound to major histocompatibility complex molecules (pMHCs). We first captured and cloned TCRα:β genes from individual cells, ensuring fidelity using a suppression PCR. We then screened TCRα:β libraries expressed in an immortalized cell line using peptide-pulsed antigen-presenting cells and sequenced activated clones to identify the cognate TCRs. Our results validated an experimental pipeline that allows large-scale repertoire datasets to be annotated with functional specificity information, facilitating the discovery of therapeutically relevant TCRs.
Publisher
Springer Science and Business Media LLC