| Literature DB >> 30700903 |
Guideng Li1,2,3, Michael T Bethune4, Stephanie Wong5, Alok V Joglekar5, Michael T Leonard5, Jessica K Wang5, Jocelyn T Kim6, Donghui Cheng7, Songming Peng8, Jesse M Zaretsky9, Yapeng Su5,8, Yicheng Luo5, James R Heath8,9,10, Antoni Ribas9,11,12,13, Owen N Witte7,9,13, David Baltimore14,15.
Abstract
T cell receptor (TCR) ligand discovery is essential for understanding and manipulating immune responses to tumors. We developed a cell-based selection platform for TCR ligand discovery that exploits a membrane transfer phenomenon called trogocytosis. We discovered that T cell membrane proteins are transferred specifically to target cells that present cognate peptide-major histocompatibility complex (MHC) molecules. Co-incubation of T cells expressing an orphan TCR with target cells collectively presenting a library of peptide-MHCs led to specific labeling of cognate target cells, enabling isolation of these target cells and sequencing of the cognate TCR ligand. We validated this method for two clinically employed TCRs and further used the platform to identify the cognate neoepitope for a subject-derived neoantigen-specific TCR. Thus, target cell trogocytosis is a robust tool for TCR ligand discovery that will be useful for studying basic tumor immunology and identifying new targets for immunotherapy.Entities:
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Year: 2019 PMID: 30700903 PMCID: PMC6719556 DOI: 10.1038/s41592-018-0305-7
Source DB: PubMed Journal: Nat Methods ISSN: 1548-7091 Impact factor: 28.547