| Literature DB >> 24166483 |
Nicola Borthwick1, Tina Ahmed1, Beatrice Ondondo2, Peter Hayes3, Annie Rose4, Umar Ebrahimsa4, Emma-Jo Hayton4, Antony Black5, Anne Bridgeman1, Maximillian Rosario6, Adrian Vs Hill7, Eleanor Berrie8, Sarah Moyle8, Nicole Frahm9, Josephine Cox3, Stefano Colloca10, Alfredo Nicosia11, Jill Gilmour3, Andrew J McMichael12, Lucy Dorrell12, Tomáš Hanke13.
Abstract
Virus diversity and escape from immune responses are the biggest challenges to the development of an effective vaccine against HIV-1. We hypothesized that T-cell vaccines targeting the most conserved regions of the HIV-1 proteome, which are common to most variants and bear fitness costs when mutated, will generate effectors that efficiently recognize and kill virus-infected cells early enough after transmission to potentially impact on HIV-1 replication and will do so more efficiently than whole protein-based T-cell vaccines. Here, we describe the first-ever administration of conserved immunogen vaccines vectored using prime-boost regimens of DNA, simian adenovirus and modified vaccinia virus Ankara to uninfected UK volunteers. The vaccine induced high levels of effector T cells that recognized virus-infected autologous CD4(+) cells and inhibited HIV-1 replication by up to 5.79 log10. The virus inhibition was mediated by both Gag- and Pol- specific effector CD8(+) T cells targeting epitopes that are typically subdominant in natural infection. These results provide proof of concept for using a vaccine to target T cells at conserved epitopes, showing that these T cells can control HIV-1 replication in vitro.Entities:
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Year: 2013 PMID: 24166483 PMCID: PMC3911893 DOI: 10.1038/mt.2013.248
Source DB: PubMed Journal: Mol Ther ISSN: 1525-0016 Impact factor: 11.454