4-1BBL Enhances CD8+ T Cell Responses Induced by Vectored Vaccines in Mice but Fails to Improve Immunogenicity in Rhesus Macaques |
| |
| Authors: | Alexandra J. Spencer Julie Furze Jared D. Honeycutt Alice Calvert Saroj Saurya Stefano Colloca David H. Wyllie Sarah C. Gilbert Migena Bregu Matthew G. Cottingham Adrian V. S. Hill |
| |
| Affiliation: | 1. The Jenner Institute, University of Oxford, Oxford, United Kingdom.; 2. Okairòs, Rome, Italy.; Federal University of São Paulo, Brazil, |
| |
| Abstract: | T cells play a central role in the immune response to many of the world’s major infectious diseases. In this study we investigated the tumour necrosis factor receptor superfamily costimulatory molecule, 4-1BBL (CD137L, TNFSF9), for its ability to increase T cell immunogenicity induced by a variety of recombinant vectored vaccines. To efficiently test this hypothesis, we assessed a number of promoters and developed a stable bi-cistronic vector expressing both the antigen and adjuvant. Co-expression of 4-1BBL, together with our model antigen TIP, was shown to increase the frequency of murine antigen-specific IFN-γ secreting CD8+ T cells in three vector platforms examined. Enhancement of the response was not limited by co-expression with the antigen, as an increase in CD8+ immunogenicity was also observed by co-administration of two vectors each expressing only the antigen or adjuvant. However, when this regimen was tested in non-human primates using a clinical malaria vaccine candidate, no adjuvant effect of 4-1BBL was observed limiting its potential use as a single adjuvant for translation into a clinical vaccine. |
| |
| Keywords: | |
|
|
