Codon-optimized filovirus DNA vaccines delivered by intramuscular electroporation protect cynomolgus macaques from lethal Ebola and Marburg virus challenges

Cynomolgus macaques were vaccinated by intramuscular electroporation with DNA plasmids expressing codon-optimized glycoprotein (GP) genes of Ebola virus (EBOV) or Marburg virus (MARV) or a combination of codon-optimized GP DNA vaccines for EBOV, MARV, Sudan virus and Ravn virus. When measured by ELI...

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Veröffentlicht in:Human vaccines & immunotherapeutics 2015-08, Vol.11 (8), p.1991-2004
Hauptverfasser: Grant-Klein, Rebecca J, Altamura, Louis A, Badger, Catherine V, Bounds, Callie E, Van Deusen, Nicole M, Kwilas, Steven A, Vu, Hong A, Warfield, Kelly L, Hooper, Jay W, Hannaman, Drew, Dupuy, Lesley C, Schmaljohn, Connie S
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Sprache:eng
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Zusammenfassung:Cynomolgus macaques were vaccinated by intramuscular electroporation with DNA plasmids expressing codon-optimized glycoprotein (GP) genes of Ebola virus (EBOV) or Marburg virus (MARV) or a combination of codon-optimized GP DNA vaccines for EBOV, MARV, Sudan virus and Ravn virus. When measured by ELISA, the individual vaccines elicited slightly higher IgG responses to EBOV or MARV than did the combination vaccines. No significant differences in immune responses of macaques given the individual or combination vaccines were measured by pseudovirion neutralization or IFN-γ ELISpot assays. Both the MARV and mixed vaccines were able to protect macaques from lethal MARV challenge (5/6 vs. 6/6). In contrast, a greater proportion of macaques vaccinated with the EBOV vaccine survived lethal EBOV challenge in comparison to those that received the mixed vaccine (5/6 vs. 1/6). EBOV challenge survivors had significantly higher pre-challenge neutralizing antibody titers than those that succumbed.
ISSN:2164-5515
2164-554X
DOI:10.1080/21645515.2015.1039757