4.5 Article

Homologous peptides derived from influenza A, B and C viruses induce variable CD8+ T cell responses with cross-reactive potential

CLINICAL & TRANSLATIONAL IMMUNOLOGY (2022)

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Journal

CLINICAL & TRANSLATIONAL IMMUNOLOGY
Volume 11, Issue 10, Pages -

Publisher

WILEY
DOI: 10.1002/cti2.1422

Keywords

CD8(+) T cell; cross-reactivity; HLA; immune response; immunodominant epitope; Influenza

Categories

Immunology

Funding

  1. Australian Research Council (ARC)
  2. National Health and Medical Research Council (NHMRC)
  3. AINSE Postgraduate Research Award
  4. Australian Government Research Training Program Scholarship
  5. NHMRC CJ Martin Fellowship [1110429]
  6. Australian Research Council DECRA [DE210101479]
  7. AINSE Early Career Researcher Grant
  8. NHMRC SRF [1159272]
  9. Australian Research Council [DE210101479] Funding Source: Australian Research Council

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This study provides a detailed characterization of the CD8(+) T cell response towards NP265_IAV and its IBV and ICV homologues, and identifies a potential vaccination target that is broad enough to cover all three influenza strains.
Objective. Influenza A, B and C viruses (IAV, IBV and ICV, respectively) circulate globally, infecting humans and causing widespread morbidity and mortality. Here, we investigate the T cell response towards an immunodominant IAV epitope, NP265-273, and its IBV and ICV homologues, presented by HLA-A*03:01 molecule expressed in similar to 4% of the global population (similar to 300 million people). Methods. We assessed the magnitude (tetramer staining) and quality of the CD8(+) T cell response (intracellular cytokine staining) towards NP265-IAV and described the T cell receptor (TCR) repertoire used to recognise this immunodominant epitope. We next assessed the immunogenicity of NP265-IAV homologue peptides from IBV and ICV and the ability of CD8(+) T cells to cross-react towards these homologous peptides. Furthermore, we determined the structures of NP265-IAV and NP323-IBV peptides in complex with HLA-A*03:01 by X-ray crystallography. Results. Our study provides a detailed characterisation of the CD8(+) T cell response towards NP265_IAV and its IBV and ICV homologues. The data revealed a diverse repertoire for NP265_IAV that is associated with superior anti-viral protection. Evidence of cross-reactivity between the three different influenza virus strain-derived epitopes was observed, indicating the discovery of a potential vaccination target that is broad enough to cover all three influenza strains. Conclusion. We show that while there is a potential to cross-protect against distinct influenza virus lineages, the T cell response was stronger against the IAV peptide than IBV or ICV, which is an important consideration when choosing targets for future vaccine design.

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