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M2e-tetramer-specific memory CD4 T cells are broadly protective against influenza infection

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  • M2e-tetramer-specific memory CD4 T cells are broadly protective against influenza infection

    Mucosal Immunol. 2017 Mar 15. doi: 10.1038/mi.2017.14. [Epub ahead of print]
    M2e-tetramer-specific memory CD4 T cells are broadly protective against influenza infection.

    Eliasson DG1, Omokanye A1, Sch?n K1, Wenzel UA1, Bernasconi V1, Bemark M1, Kolpe A2, El Bakkouri K2, Ysenbaert T2, Deng L2, Fiers W2, Saelens X2, Lycke N1.
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    Abstract

    Matrix protein 2 ectodomain (M2e) is considered an attractive component of a broadly protective, universal influenza A vaccine. Here we challenge the canonical view that antibodies against M2e are the prime effectors of protection. Intranasal immunizations of Balb/c mice with CTA1-3M2e-DD-generated M2e-specific memory CD4 T cells that were I-Ad restricted and critically protected against infection, even in the complete absence of antibodies, as observed in JhD mice. Whereas some M2e-tetramer-specific memory CD4 T cells resided in spleen and lymph nodes, the majority were lung-resident Th17 cells, that rapidly expanded upon a viral challenge infection. Indeed, immunized IL-17A-/- mice were significantly less well protected compared with wild-type mice despite exhibiting comparable antibody levels. Similarly, poor protection was also observed in congenic Balb/B (H-2b) mice, which failed to develop M2e-specific CD4 T cells, but exhibited comparable antibody levels. Lung-resident CD69+ CD103low M2e-specific memory CD4 T cells were αβ TCR+ and 50% were Th17 cells that were associated with an early influx of neutrophils after virus challenge. Adoptively transferred M2e memory CD4 T cells were strong helper T cells, which accelerated M2e- but more importantly also hemagglutinin-specific IgG production. Thus, for the first time we demonstrate that M2e-specific memory CD4 T cells are broadly protective.Mucosal Immunology advance online publication 15 March 2017. doi:10.1038/mi.2017.14.


    PMID: 28295019 DOI: 10.1038/mi.2017.14
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