Molecular Therapy: Methods & Clinical Development (Jan 2016)

Broad HIV-1 inhibition in vitro by vaccine-elicited CD8+ T cells in African adults

  • Gaudensia Mutua,
  • Bashir Farah,
  • Robert Langat,
  • Jackton Indangasi,
  • Simon Ogola,
  • Brian Onsembe,
  • Jakub T Kopycinski,
  • Peter Hayes,
  • Nicola J Borthwick,
  • Ambreen Ashraf,
  • Len Dally,
  • Burc Barin,
  • Annika Tillander,
  • Jill Gilmour,
  • Jan De Bont,
  • Alison Crook,
  • Drew Hannaman,
  • Josephine H Cox,
  • Omu Anzala,
  • Patricia E Fast,
  • Marie Reilly,
  • Kundai Chinyenze,
  • Walter Jaoko,
  • Tomáš Hanke

DOI
https://doi.org/10.1038/mtm.2016.61
Journal volume & issue
Vol. 3, no. C

Abstract

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We are developing a pan-clade HIV-1 T-cell vaccine HIVconsv, which could complement Env vaccines for prophylaxis and be a key to HIV cure. Our strategy focuses vaccine-elicited effector T-cells on functionally and structurally conserved regions (not full-length proteins and not only epitopes) of the HIV-1 proteome, which are common to most global variants and which, if mutated, cause a replicative fitness loss. Our first clinical trial in low risk HIV-1-negative adults in Oxford demonstrated the principle that naturally mostly subdominant epitopes, when taken out of the context of full-length proteins/virus and delivered by potent regimens involving combinations of simian adenovirus and poxvirus modified vaccinia virus Ankara, can induce robust CD8+ T cells of broad specificities and functions capable of inhibiting in vitro HIV-1 replication. Here and for the first time, we tested this strategy in low risk HIV-1-negative adults in Africa. We showed that the vaccines were well tolerated and induced high frequencies of broadly HIVconsv-specific plurifunctional T cells, which inhibited in vitro viruses from four major clades A, B, C, and D. Because sub-Saharan Africa is globally the region most affected by HIV-1/AIDS, trial HIV-CORE 004 represents an important stage in the path toward efficacy evaluation of this highly rational and promising vaccine strategy.