Imagen de Portada
Código QR

Immunization with Neospora caninum profilin induces limited protection and a regulatory T-cell response in mice

Profilins are actin-binding proteins that regulate the polymerization of actin filaments. In apicomplexan parasites, they are essential for invasion. Profilins also trigger the immune response of the host by activating TLRs on dendritic cells (DCs), inducing the production of pro-inflammatory cytoki...

Descripción completa

Autores principales: Mansilla, Florencia Celeste, Quintana, Maria Eugenia, Langellotti, Cecilia Ana, Wilda, Maximiliano, Martinez, Andrea, Fonzo, Adriana, Moore, Prando Dadin, Cardoso, Nancy, Capozzo, Alejandra
Formato: info:ar-repo/semantics/artículo
Lenguaje:Inglés
Publicado: 2017
Materias:
Enfermedades de los Animales
Neospora Caninum
Inmunización
Linfocitos-t
Ratón
Animal Diseases
Immunization
T-lymphocytes
Mice
Acceso en línea:http://hdl.handle.net/20.500.12123/1370
http://www.sciencedirect.com/science/article/pii/S0014489415300552
https://doi.org/10.1016/j.exppara.2015.10.008
Sumario:Profilins are actin-binding proteins that regulate the polymerization of actin filaments. In apicomplexan parasites, they are essential for invasion. Profilins also trigger the immune response of the host by activating TLRs on dendritic cells (DCs), inducing the production of pro-inflammatory cytokines. In this study we characterized for the first time the immune response and protection elicited by a vaccine based on Neospora caninum profilin in mice. Groups of eight BALB/c mice received either two doses of a recombinant N. caninum profilin expressed in Escherichia coli. (rNcPRO) or PBS, both formulated with an aqueous soy-based adjuvant enriched in TLR-agonists. Specific anti-profilin antibodies were detected in rNcPRO-vaccinated animals, mainly IgM and IgG3, which were consumed after infection. Splenocytes from rNcPRO-immunized animals proliferated after an in vitro stimulation with rNcPRO before and after challenge. An impairment of the cellular response was observed in NcPRO vaccinated and infected mice following an in vitro stimulation with native antigens of N. caninum, related to an increase in the percentage of CD4þCD25þFoxP3þ. Two out of five rNcPRO-vaccinated challenged mice were protected; they were negative for parasite DNA in the brain and showed no histopathological lesions, which were found in all PBS-vaccinated animals. As a whole, our results provide evidence of a regulatory response elicited by immunization with rNcPRO, and suggest a role of profilin in the modulation and/or evasion of immune responses against N. caninum.

Ejemplares similares