Vaccines (Jan 2020)

Synthetic DNA Vaccines Adjuvanted with pIL-33 Drive Liver-Localized T Cells and Provide Protection from <i>Plasmodium</i> Challenge in a Mouse Model

  • Sophia M. Reeder,
  • Emma L. Reuschel,
  • Mamadou A. Bah,
  • Kun Yun,
  • Nicholas J. Tursi,
  • Kevin Y. Kim,
  • Jacqueline Chu,
  • Faraz I. Zaidi,
  • Ilknur Yilmaz,
  • Robert J. Hart,
  • Benjamin Perrin,
  • Ziyang Xu,
  • Laurent Humeau,
  • David B. Weiner,
  • Ahmed S. I. Aly

DOI
https://doi.org/10.3390/vaccines8010021
Journal volume & issue
Vol. 8, no. 1
p. 21

Abstract

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The need for a malaria vaccine is indisputable. A single vaccine for Plasmodium pre-erythrocytic stages targeting the major sporozoite antigen circumsporozoite protein (CSP) has had partial success. Additionally, CD8+ T cells targeting liver-stage (LS) antigens induced by live attenuated sporozoite vaccines were associated with protection in human challenge experiments. To further evaluate protection mediated by LS antigens, we focused on exported pre-erythrocytic proteins (exported protein 1 (EXP1), profilin (PFN), exported protein 2 (EXP2), inhibitor of cysteine proteases (ICP), transmembrane protein 21 (TMP21), and upregulated in infective sporozoites-3 (UIS3)) expressed in all Plasmodium species and designed optimized, synthetic DNA (synDNA) immunogens. SynDNA antigen cocktails were tested with and without the molecular adjuvant plasmid IL-33. Immunized animals developed robust T cell responses including induction of antigen-specific liver-localized CD8+ T cells, which were enhanced by the co-delivery of plasmid IL-33. In total, 100% of mice in adjuvanted groups and 71%−88% in non-adjuvanted groups were protected from blood-stage disease following Plasmodium yoelii sporozoite challenge. This study supports the potential of synDNA LS antigens as vaccine components for malaria parasite infection.

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