Cell Reports (Apr 2020)

CD4+ T Cells Cross-Reactive with Dengue and Zika Viruses Protect against Zika Virus Infection

  • Jinsheng Wen,
  • Ying-Ting Wang,
  • Kristen M. Valentine,
  • Rúbens Prince dos Santos Alves,
  • Zhigang Xu,
  • Jose Angel Regla-Nava,
  • Annie Elong Ngono,
  • Matthew P. Young,
  • Luís C.S. Ferreira,
  • Sujan Shresta

Journal volume & issue
Vol. 31, no. 4

Abstract

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Summary: The underlying mechanisms by which prior immunity to dengue virus (DENV) affords cross-protection against the related flavivirus Zika virus (ZIKV) are poorly understood. Here, we examine the ability of DENV/ZIKV-cross-reactive CD4+ T cells to protect against versus exacerbate ZIKV infection by using a histocompatibility leukocyte antigen (HLA)-DRB1∗0101 transgenic, interferon α/β receptor-deficient mouse model that supports robust DENV and ZIKV replication. By mapping the HLA-DRB1∗0101-restricted T cell response, we identify DENV/ZIKV-cross-reactive CD4+ T cell epitopes that stimulate interferon gamma (IFNγ) and/or tumor necrosis factor (TNF) production. Vaccination of naive HLA-DRB1∗0101 transgenic mice with these peptides induces a CD4+ T cell response sufficient to reduce tissue viral burden following ZIKV infection. Notably, this protective response requires IFNγ and/or TNF secretion but not anti-ZIKV immunoglobulin G (IgG) production. Thus, DENV/ZIKV-cross-reactive CD4+ T cells producing canonical Th1 cytokines can suppress ZIKV replication in an antibody-independent manner. These results may have important implications for increasing the efficacy and safety of DENV/ZIKV vaccines and for developing pan-flavivirus vaccines. : Wen et al. show that dengue and Zika virus cross-reactive CD4+ T cells reduce Zika viral burden in interferon α/β receptor-deficient HLA-DRB1∗0101 transgenic mice in an IFNγ- or TNF-dependent, antibody-independent manner. Keywords: dengue virus, Zika virus, CD4+, T cell, Th1, cross-protection, cross-reactive, peptide, mouse, IFNγ, TNF