Chimeric calicivirus-like particles elicit protective anti-viral cytotoxic responses without adjuvant

E. Crisci, H. Almanza, I. Mena, L. Córdoba, E. Gómez-Casado, J. R. Castón, L. Fraile, J. Bárcena, M. Montoya

    Producció científica: Contribució a una revistaArticleRecercaAvaluat per experts

    28 Cites (Scopus)

    Resum

    We have analyzed the potential of virus-like particles (VLPs) from rabbit hemorrhagic disease virus (RHDV) as a delivery system for foreign T cell epitopes. To accomplish this goal, we generated chimeric RHDV-VLPs incorporating a CD8+ T cell epitope (SIINFEKL) derived from chicken ovalbumin (OVA). The OVA epitope was inserted in the capsid protein (VP60) of RHDV at two different locations: 1) the N-terminus, predicted to be facing to the inner core of the VLPs, and 2) a novel insertion site predicted to be located within an exposed loop. Both constructions correctly assembled into VLPs. In vitro, the chimeric VLPs activated dendritic cells for TNF-α secretion and they were processed and presented to specific T cells. In vivo, mice immunized with the chimeric VLPs without adjuvant were able to induce specific cellular responses mediated by cytotoxic and memory T cells. More importantly, immunization with chimeric VLPs was able to resolve an infection by a recombinant vaccinia virus expressing OVA protein. © 2009 Elsevier Inc. All rights reserved.
    Idioma originalEnglish
    Pàgines (de-a)303-312
    RevistaVirology
    Volum387
    Número2
    DOIs
    Estat de la publicacióPublicada - 10 de maig 2009

    Fingerprint

    Navegar pels temes de recerca de 'Chimeric calicivirus-like particles elicit protective anti-viral cytotoxic responses without adjuvant'. Junts formen un fingerprint únic.

    Com citar-ho