Artículo
Evaluation of the immune response elicited by vaccination with viral vectors encoding FMDV capsid proteins and boosted with inactivated virus
Romanutti, Carina
; D'antuono, Alejandra Lorena
; Palacios, Carlos Adolfo
; Quattrocchi, Valeria; Zamorano, Patricia Ines
; la Torre, Jose Leonardo
; Mattion, Nora Marta
Fecha de publicación:
30/08/2013
Editorial:
Elsevier
Revista:
Veterinary Microbiology
ISSN:
0378-1135
Idioma:
Inglés
Tipo de recurso:
Artículo publicado
Clasificación temática:
Resumen
The aim of the present study was to assess the effect of introducing a priming step with replication-defective viral vectors encoding the capsid proteins of FMDV, followed by a boost with killed virus vaccines, using a suitable BALB/c mice model. Additionally, the immune response to other combined vector immunization regimens was studied. For this purpose, we analyzed different prime-boost immunizations with recombinant adenovirus (Ad), herpesvirus amplicons (Hs) and/or killed virus (KV) vaccines. The highest antibody titers were found in the group that received two doses of adjuvanted KV (P < 0.002). Antibody titers were higher in those groups receiving a mixed regimen of vectors, compared to immunization with either vector alone (P < 0.0001). Priming with any of the viral vectors induced a shift of the cytokine balance toward a Th1 type immune response regardless of the delivery system used for boosting. The highest IgG1 titer was induced by two doses of adjuvanted KV (P = 0.0002) and the highest IgG2a titer corresponded to the group primed with Ad and boosted with KV (P = 0.01). Re-stimulation of all groups of mice with 0.5 mg of inactivated virus five months later resulted in a fast increase of antibody titers in all the groups tested. After virus stimulation, antibody titers in the groups that received KV alone or Ad prime-KV boost, were indistinguishable (P = 0.800). Protection from challenge was similar (75%) in the groups of animals that received Ad prime-Hs boost or Ad prime-KV boost, or two doses of oil-adjuvanted KV. The data presented in this study suggest that sequential immunization with viral vectors-based vaccines combined with protein-based vaccines have the potential to enhance the quality of the immune response against FMDV.
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Articulos(ICT - MILSTEIN)
Articulos de INST.DE CS. Y TECNOLOGIA "DR. CESAR MILSTEIN"
Articulos de INST.DE CS. Y TECNOLOGIA "DR. CESAR MILSTEIN"
Citación
Romanutti, Carina; D'antuono, Alejandra Lorena; Palacios, Carlos Adolfo; Quattrocchi, Valeria; Zamorano, Patricia Ines; et al.; Evaluation of the immune response elicited by vaccination with viral vectors encoding FMDV capsid proteins and boosted with inactivated virus; Elsevier; Veterinary Microbiology; 165; 3-4; 30-8-2013; 333-340
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