A Diverse Lipid Antigen-Specific TCR Repertoire Is Clonally Expanded during Active Tuberculosis

Human T cells that recognize lipid Ags presented by highly conserved CD1 proteins often express semi-invariant TCRs, but the true diversity of lipid Ag-specific TCRs remains unknown. We use CD1b tetramers and high-throughput immunosequencing to analyze thousands of TCRs from ex vivo-sorted or in vit...

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Veröffentlicht in:The Journal of immunology (1950) 2018-08, Vol.201 (3), p.888-896
Hauptverfasser: DeWitt, William S, Yu, Krystle K Q, Wilburn, Damien B, Sherwood, Anna, Vignali, Marissa, Day, Cheryl L, Scriba, Thomas J, Robins, Harlan S, Swanson, Willie J, Emerson, Ryan O, Bradley, Philip H, Seshadri, Chetan
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Sprache:eng
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Zusammenfassung:Human T cells that recognize lipid Ags presented by highly conserved CD1 proteins often express semi-invariant TCRs, but the true diversity of lipid Ag-specific TCRs remains unknown. We use CD1b tetramers and high-throughput immunosequencing to analyze thousands of TCRs from ex vivo-sorted or in vitro-expanded T cells specific for the mycobacterial lipid Ag, glucose monomycolate. Our results reveal a surprisingly diverse repertoire resulting from editing of germline-encoded gene rearrangements analogous to MHC-restricted TCRs. We used a distance-based metric (TCRDist) to show how this diverse TCR repertoire builds upon previously reported conserved motifs by including subject-specific TCRs. In a South African cohort, we show that TCRDist can identify clonal expansion of diverse glucose monomycolate-specific TCRs and accurately distinguish patients with active tuberculosis from control subjects. These data suggest that similar mechanisms govern the selection and expansion of peptide and lipid Ag-specific T cells despite the nonpolymorphic nature of CD1.
ISSN:0022-1767
1550-6606
DOI:10.4049/jimmunol.1800186