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Polyfunctional CD4+ T cell responses to a set of pathogenic arenaviruses provide broad population coverage |
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| Authors: | Maya F Kotturi Jason Botten Matt Maybeno John Sidney Jean Glenn Huynh-Hoa Bui Carla Oseroff Shane Crotty Bjoern Peters Howard Grey Daniel M Altmann Michael J Buchmeier Alessandro Sette |
| Institution: | 1. Division of Vaccine Discovery, La Jolla Ins7titute for Allergy and Immunology, 9420 Athena Circle, La Jolla, California, 92037, USA 2. Department of Medicine, The University of Vermont College of Medicine, 89 Beaumont Avenue, Burlington, Vermont, 05405-0068, USA 3. Department of Infectious Diseases and Immunity, Faculty of Medicine, Imperial College, London W12, 0NN, UK 4. Department of Molecular Biology and Biochemistry, University of California, 3205 McGaugh Hall, Irvine, California, 92697-3900, USA 5. Department of Community and Environmental Medicine, University of California, 3205 McGaugh Hall, Irvine, California, 92697-3900, USA |
| Abstract: | BackgroundSeveral arenaviruses cause severe hemorrhagic fever and aseptic meningitis in humans for which no licensed vaccines are available. A major obstacle for vaccine development is pathogen heterogeneity within the Arenaviridae family. Evidence in animal models and humans indicate that T cell and antibody-mediated immunity play important roles in controlling arenavirus infection and replication. Because CD4+ T cells are needed for optimal CD8+ T cell responses and to provide cognate help for B cells, knowledge of epitopes recognized by CD4+ T cells is critical to the development of an effective vaccine strategy against arenaviruses. Thus, the goal of the present study was to define and characterize CD4+ T cell responses from a broad repertoire of pathogenic arenaviruses (including lymphocytic choriomeningitis, Lassa, Guanarito, Junin, Machupo, Sabia, and Whitewater Arroyo viruses) and to provide determinants with the potential to be incorporated into a multivalent vaccine strategy.ResultsBy inoculating HLA-DRB1*0101 transgenic mice with a panel of recombinant vaccinia viruses, each expressing a single arenavirus antigen, we identified 37 human HLA-DRB1*0101-restricted CD4+ T cell epitopes from the 7 antigenically distinct arenaviruses. We showed that the arenavirus-specific CD4+ T cell epitopes are capable of eliciting T cells with a propensity to provide help and protection through CD40L and polyfunctional cytokine expression. Importantly, we demonstrated that the set of identified CD4+ T cell epitopes provides broad, non-ethnically biased population coverage of all 7 arenavirus species targeted by our studies.ConclusionsThe identification of CD4+ T cell epitopes, with promiscuous binding properties, derived from 7 different arenavirus species will aid in the development of a T cell-based vaccine strategy with the potential to target a broad range of ethnicities within the general population and to protect against both Old and New World arenavirus infection. |
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