AUTHOR=de León Patricia , Cañas-Arranz Rodrigo , Defaus Sira , Torres Elisa , Forner Mar , Bustos María J. , Revilla Concepción , Dominguez Javier , Andreu David , Blanco Esther , Sobrino Francisco 

TITLE=Swine T-Cells and Specific Antibodies Evoked by Peptide Dendrimers Displaying Different FMDV T-Cell Epitopes

JOURNAL=Frontiers in Immunology

VOLUME=11

YEAR=2021

URL=https://www.frontiersin.org/journals/immunology/articles/10.3389/fimmu.2020.621537

DOI=10.3389/fimmu.2020.621537

ISSN=1664-3224

ABSTRACT=<p>Dendrimeric peptide constructs based on a lysine core that comprises both B- and T-cell epitopes of foot-and-mouth disease virus (FMDV) have proven a successful strategy for the development of FMD vaccines. Specifically, B<sub>2</sub>T dendrimers displaying two copies of the major type O FMDV antigenic B-cell epitope located on the virus capsid [VP1 (140–158)], covalently linked to a heterotypic T-cell epitope from either non-structural protein 3A [3A (21–35)] or 3D [3D (56–70)], named B<sub>2</sub>T-3A and B<sub>2</sub>T-3D, respectively, elicit high levels of neutralizing antibodies (nAbs) and IFN-γ-producing cells in pigs. To assess whether the inclusion and orientation of T-3A and T-3D T-cell epitopes in a single molecule could modulate immunogenicity, dendrimers with T epitopes juxtaposed in both possible orientations, i.e., constructs B<sub>2</sub>TT-3A3D and B<sub>2</sub>TT-3D3A, were made and tested in pigs. Both dendrimers elicited high nAbs titers that broadly neutralized type O FMDVs, although B<sub>2</sub>TT-3D3A did not respond to boosting, and induced lower IgGs titers, in particular IgG2, than B<sub>2</sub>TT-3A3D. Pigs immunized with B<sub>2,</sub> a control dendrimer displaying two B-cell epitope copies and no T-cell epitope, gave no nABs, confirming T-3A and T-3D as T helper epitopes. The T-3D peptide was found to be an immunodominant, as it produced more IFN-γ expressing cells than T-3A in the <italic>in vitro</italic> recall assay. Besides, in pigs immunized with the different dendrimeric peptides, CD4<sup>+</sup> T-cells were the major subset contributing to IFN-γ expression upon <italic>in vitro</italic> recall, and depletion of CD4<sup>+</sup> cells from PBMCs abolished the production of this cytokine. Most CD4<sup>+</sup>IFN-γ<sup>+</sup> cells showed a memory (CD4<sup>+</sup>2E3<sup>−</sup>) and a multifunctional phenotype, as they expressed both IFN-γ and TNF-α, suggesting that the peptides induced a potent Th1 pro-inflammatory response. Furthermore, not only the presence, but also the orientation of T-cell epitopes influenced the T-cell response, as B<sub>2</sub>TT-3D3A and B<sub>2</sub> groups had fewer cells expressing both cytokines. These results help understand how B<sub>2</sub>T-type dendrimers triggers T-cell populations, highlighting their potential as next-generation FMD vaccines.</p>