Mtb HLA-E-tetramer-sorted CD8+ T cells have a diverse TCR repertoire

结核分枝杆菌HLA-E四聚体分选的CD8+ T细胞具有多样化的TCR库

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作者:Linda Voogd ,Anne M H F Drittij ,Calinda K E Dingenouts ,Kees L M C Franken ,Vincent van Unen ,Krista E van Meijgaarden ,Paula Ruibal ,Renate S Hagedoorn ,Judith A Leitner ,Peter Steinberger ,Mirjam H M Heemskerk ,Mark M Davis ,Thomas J Scriba ,Tom H M Ottenhoff ,Simone A Joosten

Abstract

HLA-E molecules can present self- and pathogen-derived peptides to both natural killer (NK) cells and T cells. T cells that recognize HLA-E peptides via their T cell receptor (TCR) are termed donor-unrestricted T cells due to restricted allelic variation of HLA-E. The composition and repertoire of HLA-E TCRs is not known so far. We performed TCR sequencing on CD8+ T cells from 21 individuals recognizing HLA-E tetramers (TMs) folded with two Mtb-HLA-E-restricted peptides. We sorted HLA-E Mtb TM+ and TM- CD8+ T cells directly ex vivo and performed bulk RNA-sequencing and single-cell TCR sequencing. The identified TCR repertoire was diverse and showed no conservation between and within individuals. TCRs selected from our single-cell TCR sequencing data could be activated upon HLA-E/peptide stimulation, although not robust, reflecting potentially weak interactions between HLA-E peptide complexes and TCRs. Thus, HLA-E-Mtb-specific T cells have a highly diverse TCR repertoire.

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