npj Vaccines (Mar 2021)

A CCHFV DNA vaccine protects against heterologous challenge and establishes GP38 as immunorelevant in mice

  • John J. Suschak,
  • Joseph W. Golden,
  • Collin J. Fitzpatrick,
  • Charles J. Shoemaker,
  • Catherine V. Badger,
  • Connie S. Schmaljohn,
  • Aura R. Garrison

DOI
https://doi.org/10.1038/s41541-021-00293-9
Journal volume & issue
Vol. 6, no. 1
pp. 1 – 11

Abstract

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Abstract Crimean-Congo hemorrhagic fever virus (CCHFV) is a tick-borne virus that causes severe hemorrhagic fever disease in humans. Currently, no licensed CCHF vaccines exist, and the protective epitopes remain unclear. Previously, we tested a DNA vaccine expressing the M-segment glycoprotein precursor gene of the laboratory CCHFV strain IbAr 10200 (CCHFV-M10200). CCHFV-M10200 provided >60% protection against homologous CCHFV-IbAr 10200 challenge in mice. Here, we report that increasing the dose of CCHFV-M10200 provides complete protection from homologous CCHFV challenge in mice, and significant (80%) protection from challenge with the clinically relevant heterologous strain CCHFV-Afg09-2990. We also report complete protection from CCHFV-Afg09-2990 challenge following vaccination with a CCHFV-Afg09-2990 M-segment DNA vaccine (CCHFV-MAfg09). Finally, we show that the non-structural M-segment protein, GP38, influences CCHF vaccine immunogenicity and provides significant protection from homologous CCHFV challenge. Our results demonstrate that M-segment DNA vaccines elicit protective CCHF immunity and further illustrate the immunorelevance of GP38.