TY - JOUR
T1 - A T-cell epitope on NS3 non-structural protein enhances the B and T cell responses elicited by dendrimeric constructions against CSFV in domestic pigs
AU - Tarradas, Joan
AU - Monsó, Marta
AU - Fraile, Lorenzo
AU - de la Torre, Beatriz G.
AU - Muñoz, Marta
AU - Rosell, Rosa
AU - Riquelme, Cristina
AU - Pérez, Lester Josué
AU - Nofrarías, Miquel
AU - Domingo, Mariano
AU - Sobrino, Francisco
AU - Andreu, David
AU - Ganges, Llilianne
N1 - Funding Information:
We thank Iván Cordón and David Solanes for their help in the animal facilities and SEPPIC for the adjuvant. This research was primarily supported by a coordinated grant BIO2008-04487-C03-01 (CBMSO), BIO2008-04487-C03-02 (UPF) and BIO2008-04487-C03-03 (CReSA) from the Spanish Ministry of Science and Innovation (MICINN) . Work at CreSA and CBMSO was additionally supported by Consolider Ingenio 2011 CSD2006-0007 from MICINN. Institutional grants from Fundación Areces for CBMSO and from Generalitat de Catalunya ( SGR2009-492 ) for UPF also helped to support this research.
PY - 2012/11/15
Y1 - 2012/11/15
N2 - It has been recently reported by our group that dendrimeric constructs combining B- and T-cell epitopes from classical swine fever virus (CSFV) provided partial protection against experimental infection. This research evaluated four newly designed constructions while taking into account our previous work, including the direct implication that a T-cell epitope from the NS3 protein contributes to the generation of the immune response against CSFV. To this end, the dendrimeric constructions, including either this NS3 T-cell epitope alone or two different B-cell epitopes without this T-cell epitope, were used to immunise pigs. Thus, construct 1, containing the NS3 T-cell epitope and four copies of a previously described B-cell epitope, significantly reduced the clinical scores and RNA viral loads after challenge relative to the control group. In three out of six animals in this group, vaccination achieved partial protection and was associated with IFN-gamma producing-cells and neutralising antibodies. In contrast, the pigs immunised with construct 2, again with four copies of the B epitope of construct 1 but lacking the T-cell motif, developed more severe clinical signs. Finally, the additional constructs 3 and 4 included four copies of a B epitope that was different from the epitope used in constructs 1 and 2 with or without the abovementioned NS3 T-cell epitope, respectively. Pigs immunised with these latter constructs developed low levels of peptide-specific antibodies that correlated with equally low levels of cellular responses, an absence of neutralising antibodies and a lack of protection. Even so, the clinical scores in the first week after the challenge were less severe for animals vaccinated with construct 3 than for those given construct 4. Our results confirm the relevant role of the B-cell epitope in residues 694-712 of the glycoprotein E2 (which is used in both constructs 1 and 2) for protection against CSFV, as well as the appropriateness of the newly used NS3 peptide as a specific T-cell epitope in domestic pigs.
AB - It has been recently reported by our group that dendrimeric constructs combining B- and T-cell epitopes from classical swine fever virus (CSFV) provided partial protection against experimental infection. This research evaluated four newly designed constructions while taking into account our previous work, including the direct implication that a T-cell epitope from the NS3 protein contributes to the generation of the immune response against CSFV. To this end, the dendrimeric constructions, including either this NS3 T-cell epitope alone or two different B-cell epitopes without this T-cell epitope, were used to immunise pigs. Thus, construct 1, containing the NS3 T-cell epitope and four copies of a previously described B-cell epitope, significantly reduced the clinical scores and RNA viral loads after challenge relative to the control group. In three out of six animals in this group, vaccination achieved partial protection and was associated with IFN-gamma producing-cells and neutralising antibodies. In contrast, the pigs immunised with construct 2, again with four copies of the B epitope of construct 1 but lacking the T-cell motif, developed more severe clinical signs. Finally, the additional constructs 3 and 4 included four copies of a B epitope that was different from the epitope used in constructs 1 and 2 with or without the abovementioned NS3 T-cell epitope, respectively. Pigs immunised with these latter constructs developed low levels of peptide-specific antibodies that correlated with equally low levels of cellular responses, an absence of neutralising antibodies and a lack of protection. Even so, the clinical scores in the first week after the challenge were less severe for animals vaccinated with construct 3 than for those given construct 4. Our results confirm the relevant role of the B-cell epitope in residues 694-712 of the glycoprotein E2 (which is used in both constructs 1 and 2) for protection against CSFV, as well as the appropriateness of the newly used NS3 peptide as a specific T-cell epitope in domestic pigs.
KW - Cellular and humoural immune response
KW - Classical swine fever virus
KW - Dendrimeric peptide vaccine
KW - Epitopes
KW - Marker (DIVA) vaccine
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U2 - 10.1016/j.vetimm.2012.08.006
DO - 10.1016/j.vetimm.2012.08.006
M3 - Article
C2 - 22959286
AN - SCOPUS:84867332186
SN - 0165-2427
VL - 150
SP - 36
EP - 46
JO - Veterinary Immunology and Immunopathology
JF - Veterinary Immunology and Immunopathology
IS - 1-2
ER -