Narrowing of Human Influenza A Virus-Specific T Cell Receptor α and β Repertoires with Increasing Age

Gil, Anna; Yassai, Maryam; Naumov, Yuri N.; Selin, Liisa K.

doi:10.1128/jvi.03020-14

Cited by 75 publications

(96 citation statements)

References 53 publications

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“…Moreover, contraction was caused by a preferential loss of infrequent T cell clones, consistent with the interpretation of greater selection of dominant T cell specificities. A similar observation of contraction at the epitope level has been made for the repertoire of influenza-specific CD8 T cells in older individuals suggesting that age may be a contributing factor (20). The clinical relevance of repertoire diversity has been shown for CMV infection, where the number of different TCRs reactive to a CMV peptide was more important for effective control of viral latency than their frequencies (17).…”

Section: Discussionsupporting

confidence: 68%

“…In general, during infection or vaccination, epitope-specific naive CD8 T cells are recruited into the memory compartment. However, deterministic selection mechanisms cause skewed clonal size distributions that further increase in chronic infections and recall responses (19, 20). These observations raise the question of whether vaccination induces a contraction of the virus specific repertoire owing to the disproportionate expansion of dominant clones.…”

Section: Introductionmentioning

confidence: 99%

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Diversification of the antigen-specific T cell receptor repertoire after varicella zoster vaccination

et al. 2016

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Diversity and size of the antigen-specific T cell receptor (TCR) repertoire are two critical determinants for successful control of chronic infection. Varicella zoster virus (VZV) that establishes latency during childhood is able to escape control mechanisms, in particular with increasing age. We examined the TCR diversity of VZV-reactive CD4 T cells in individuals older than 50 years by studying three identical twin pairs and three unrelated individuals before and after vaccination with live attenuated VZV. While all individuals had a small number of dominant T cell clones, the breadth of the VZV-specific repertoire differed markedly. A genetic influence was seen for the sharing of individual TCR sequences from antigen-reactive cells, but not for repertoire richness or the selection of dominant clones. VZV vaccination favored the expansion of infrequent VZV antigen-reactive TCRs including those from naïve T cells with lesser boosting of dominant T cell clones. Thus, vaccination does not reinforce the in vivo selection occurred during chronic infection but leads to a diversification of the VZV-reactive T cell repertoire. However, a single booster immunization seems insufficient to establish new clonal dominance. Our results suggest that repertoire analysis of antigen-specific TCRs can be an important read-out to assess whether a vaccination was able to generate memory cells in clonal sizes that are necessary for immune protection.

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Section: Discussionsupporting

confidence: 68%

Section: Introductionmentioning

confidence: 99%

Diversification of the antigen-specific T cell receptor repertoire after varicella zoster vaccination

et al. 2016

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“…These numbers are in line with estimates of the precursor frequency of naïve T cells recognizing various antigenic peptides in other mouse and human models 38–40 . Overall diversity measures for this repertoire were at the upper end of the range of values previously reported for other viral epitope-specific responses 19,32,41,42 . As previously reported, a single public TRBV gene segment (TRBV19) with restricted CDR3β motif (xRS/Ax) (Group I) dominated the HLA-A2/M1 response, representing in this cohort ~50% (range 15–72%) of the responding CD8 T cells and 12–55% of the unique sequences.…”

Section: Discussionsupporting

confidence: 51%

“…We then used HLA-A2/M1 dextramer to sort antigen-specific cells before isolating cDNA for NGS analysis of the TRAV and TRBV repertoires. Previous approaches using 5’-RACE PCR 12 , or using individual primers for each TRAV or TRBV gene and then subcloning 32 , were not designed to exhaustively sample the repertoire, and on average identified 20–100 unique TCRα or TCRβ clonotypes specific to HLA-A2/M1 in any donor, usually examining either TRAV or TRBV repertoire but not both 11,12,32 . Using the ex vivo expansion/NGS strategy we gained a greater appreciation of the complete M1-specific TCR repertoire.…”

Section: Resultsmentioning

confidence: 99%

Broad TCR repertoire and diverse structural solutions for recognition of an immunodominant CD8+ T cell epitope

Song

Gil

Mishra

et al. 2017

Nat Struct Mol Biol

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121

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A keystone of antiviral immunity is CD8 T-cell recognition of viral peptides bound to MHC-I proteins. The recognition mode of individual T cell receptors (TCRs) has been studied in some detail, but how TCR variation functions in providing a robust response to viral antigen is unclear. The influenza M1 epitope is an immunodominant target of CD8 T cells helping to control influenza in HLA-A2+ individuals. Here, we show that many distinct TCRs are used by CD8 T cells to recognize HLA-A2/M1, encoding different structural solutions to the problem of specifically recognizing a relatively featureless peptide antigen. The vast majority of responding TCRs target small clefts between peptide and MHC. These broad repertoires lead to plasticity in antigen recognition and protection against T cell clonal loss and viral escape.

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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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Narrowing of Human Influenza A Virus-Specific T Cell Receptor α and β Repertoires with Increasing Age

Cited by 75 publications

References 53 publications

Diversification of the antigen-specific T cell receptor repertoire after varicella zoster vaccination

Diversification of the antigen-specific T cell receptor repertoire after varicella zoster vaccination

Broad TCR repertoire and diverse structural solutions for recognition of an immunodominant CD8+ T cell epitope

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

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