Nontoxic outer membrane vesicles efficiently increase the efficacy of an influenza vaccine in mice and ferrets

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Title
Nontoxic outer membrane vesicles efficiently increase the efficacy of an influenza vaccine in mice and ferrets
Author(s)
S M Shin; E J Song; D Song; Tae Young Lee; Doo-Jin Kim; J H Nam; Dae Gwin Jeong; C K Lee; S H Kim; J K Kim
Bibliographic Citation
Vaccine, vol. 35, no. 30, pp. 3741-3748
Publication Year
2017
Abstract
In this study, we developed a further-modified outer membrane vesicle (fmOMV) from the ΔmsbB/ΔpagP mutant of Escherichia coli transformed with the plasmid, pLpxF, in order to use it as an adjuvant for pandemic H1N1 (pH1N1) influenza vaccine. We evaluated the efficacy of the pH1N1 influenza vaccine containing the fmOMV in animal models as compared to the commercial adjuvants, alum or AddaVaxTM. The fmOMV-adjuvanted pH1N1 influenza vaccine induced a significant increase in the humoral immunity; however, this effect was less than that of the AddaVaxTM. The fmOMV-adjuvanted vaccine displayed pronounced an enhanced protective efficacy with increased T cell immune response and reduced the viral load in the lungs of the infected mice after challenging them with a lethal dose of the homologous virus. Moreover, it resulted in a significantly higher cross-protection against heterologous virus challenge than that of the pH1N1 vaccine with alum or with no adjuvants. In ferrets, the fmOMV-adjuvanted vaccine elicited a superior antibody response based on the HI titer and efficiently protected the animals from the lethal viral challenges. Taken together, the nontoxic fmOMV could be a promising adjuvant for inducing robust T cell priming into the pH1N1 vaccine and might be broadly applicable to the development of preventive measures against influenza virus infection.
Keyword
AdjuvantfmOMVInfluenzaPandemicT cell
ISSN
0264-410X
Publisher
Elsevier
Full Text Link
http://dx.doi.org/10.1016/j.vaccine.2017.05.053
Type
Article
Appears in Collections:
Division of Research on National Challenges > Infectious Disease Research Center > 1. Journal Articles
Division of Research on National Challenges > Bionanotechnology Research Center > 1. Journal Articles
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