Molecular basis for universal HLA-A*0201–restricted CD8
            <sup>+</sup>
            T-cell immunity against influenza viruses

Valkenburg, Sophie A.; Josephs, Tracy M.; Clemens, E. Bridie; Grant, Emma J.; Nguyen, Thi H. O.; Wang, George; Price, David A.; Miller, Adrian; Tong, Steven Y. C.; Thomas, Paul G.; Doherty, Peter C.; Rossjohn, Jamie; Gras, Stéphanie; Kedzierska, Katherine

doi:10.1073/pnas.1603106113

Cited by 101 publications

(205 citation statements)

References 41 publications

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“…S1a). From the analysed cells, we identified new as well as previously described22232930 Flu MP 58-66 -specific T cell receptor chains (see Supplementary Table S1). We noted inter-individual sharing of TCR α-chains among the analysed Flu-specific cells (Supplementary Fig.…”

Section: Resultsmentioning

confidence: 99%

CD8+ T cells specific for the islet autoantigen IGRP are restricted in their T cell receptor chain usage

Fuchs

Eugster

Dietz

et al. 2017

Sci Rep

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CD8+ T cells directed against beta cell autoantigens are considered relevant for the pathogenesis of type 1 diabetes. Using single cell T cell receptor sequencing of CD8+ T cells specific for the IGRP265-273 epitope, we examined whether there was expansion of clonotypes and sharing of T cell receptor chains in autoreactive CD8+ T cell repertoires. HLA-A*0201 positive type 1 diabetes patients (n = 19) and controls (n = 18) were analysed. TCR α- and β-chain sequences of 418 patient-derived IGRP265-273-multimer+ CD8+ T cells representing 48 clonotypes were obtained. Expanded populations of IGRP265-273-specific CD8+ T cells with dominant clonotypes that had TCR α-chains shared across patients were observed. The SGGSNYKLTF motif corresponding to TRAJ53 was contained in 384 (91.9%) cells, and in 20 (41.7%) patient-derived clonotypes. TRAJ53 together with TRAV29/DV5 was found in 15 (31.3%) clonotypes. Using next generation TCR α-chain sequencing, we found enrichment of one of these TCR α-chains in the memory CD8+ T cells of patients as compared to healthy controls. CD8+ T cell clones bearing the enriched motifs mediated antigen-specific target cell lysis. We provide the first evidence for restriction of T cell receptor motifs in the alpha chain of human CD8+ T cells with specificity to a beta cell antigen.

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Section: Resultsmentioning

confidence: 99%

CD8+ T cells specific for the islet autoantigen IGRP are restricted in their T cell receptor chain usage

Fuchs

Eugster

Dietz

et al. 2017

Sci Rep

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“…Assessment of cell division revealed that all memory CD8 + T cell subsets were capable of undergoing in vitro expansion with, on average, 60%-70% of cells within each subset undergoing at least 1 division after 10 days of culture ( Figure 3, B and C). A comparison of the effector function of the divided cells following a brief restimulation revealed that, across all the subsets, 70%-85% of the divided cells could generate IFN-γ and 80%-90% could synthesize TNF-α, reflecting that the progeny of each of the memory CD8 + T cells subsets had supe- (5,16). As predicted, CD8 + T cells directed at distinct epitopes displayed different biases in TCR-β variable (TRBV) and TCR-α variable (TRAV) usage as well as different lengths of complementarity-determining region 3α (CDR3α) and CDR3β loops ( Figure 5).…”

Section: Enrichment Of Influenza-specific Cd8mentioning

confidence: 99%

Influenza-specific lung-resident memory T cells are proliferative and polyfunctional and maintain diverse TCR profiles

Pizzolla

Nguyen

Sant

et al. 2018

Journal of Clinical Investigation

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“…EBV-and herpes simplex virus-specific clones have been shown to also react to allogeneic HLA in humans, particularly within the CD8 compartment (21,(61)(62)(63)(64)(65); it has even been suggested that nearly half of the TCRs specific to a given virus may also have alloreactivity (66). Furthermore, these viral peptide-specific TCRs may have "public" sequences shared between individuals with the same presenting HLA allele (67)(68)(69)(70). Notably, cytokine production and other measures of T cell function are not always identical in response to viral antigen and cross-reactive HLA alloantigens (21), perhaps because of differing TCR affinities for different ligands.…”

Section: Methods For Measuring the Alloresponsementioning

confidence: 99%

Alloimmune T cells in transplantation

DeWolf¹,

Sykes²

2017

Journal of Clinical Investigation

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Molecular basis for universal HLA-A*0201–restricted CD8 ⁺ T-cell immunity against influenza viruses

Cited by 101 publications

References 41 publications

CD8+ T cells specific for the islet autoantigen IGRP are restricted in their T cell receptor chain usage

CD8+ T cells specific for the islet autoantigen IGRP are restricted in their T cell receptor chain usage

Influenza-specific lung-resident memory T cells are proliferative and polyfunctional and maintain diverse TCR profiles

Alloimmune T cells in transplantation

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Molecular basis for universal HLA-A*0201–restricted CD8 + T-cell immunity against influenza viruses

Cited by 101 publications

References 41 publications

CD8+ T cells specific for the islet autoantigen IGRP are restricted in their T cell receptor chain usage

CD8+ T cells specific for the islet autoantigen IGRP are restricted in their T cell receptor chain usage

Influenza-specific lung-resident memory T cells are proliferative and polyfunctional and maintain diverse TCR profiles

Alloimmune T cells in transplantation

Contact Info

Product

Resources

About

Molecular basis for universal HLA-A*0201–restricted CD8 ⁺ T-cell immunity against influenza viruses