High-throughput and high-dimensional single-cell analysis of antigen-specific CD8+ T cells

被引:0
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作者
Ke-Yue Ma
Alexandra A. Schonnesen
Chenfeng He
Amanda Y. Xia
Eric Sun
Eunise Chen
Katherine R. Sebastian
Yu-Wan Guo
Robert Balderas
Mrinalini Kulkarni-Date
Ning Jiang
机构
[1] The University of Texas at Austin,Interdisciplinary Life Sciences Graduate Programs
[2] The University of Texas at Austin,Department of Biomedical Engineering
[3] The University of Texas atAustin,Department of Molecular Biosciences
[4] The University of Texas at Austin,Department of Nutritional Sciences
[5] The University of Texas at Austin,Department of Internal Medicine, Dell Medical School
[6] The University of Texas at Austin,McKetta Department of Chemical Engineering
[7] University of Pennsylvania,Department of Bioengineering
[8] Becton Dickinson,Department of Oncology, Dell Medical School
[9] The University of Texas at Austin,Institute for Immunology
[10] University of Pennsylvania Perelman School of Medicine,undefined
来源
Nature Immunology | 2021年 / 22卷
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摘要
Although critical to T cell function, antigen specificity is often omitted in high-throughput multiomics-based T cell profiling due to technical challenges. We describe a high-dimensional, tetramer-associated T cell antigen receptor (TCR) sequencing (TetTCR-SeqHD) method to simultaneously profile cognate antigen specificities, TCR sequences, targeted gene expression and surface-protein expression from tens of thousands of single cells. Using human polyclonal CD8+ T cells with known antigen specificity and TCR sequences, we demonstrate over 98% precision for detecting the correct antigen specificity. We also evaluate gene expression and phenotypic differences among antigen-specific CD8+ T cells and characterize phenotype signatures of influenza- and Epstein–Barr virus-specific CD8+ T cells that are unique to their pathogen targets. Moreover, with the high-throughput capacity of profiling hundreds of antigens simultaneously, we apply TetTCR-SeqHD to identify antigens that preferentially enrich cognate CD8+ T cells in patients with type 1 diabetes compared to healthy controls and discover a TCR that cross-reacts with diabetes-related and microbiome antigens. TetTCR-SeqHD is a powerful approach for profiling T cell responses in humans and mice.
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页码:1590 / 1598
页数:8
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