PLoS ONE (Jan 2013)

Gag-positive reservoir cells are susceptible to HIV-specific cytotoxic T lymphocyte mediated clearance in vitro and can be detected in vivo [corrected].

  • Erin H Graf,
  • Matthew J Pace,
  • Bennett A Peterson,
  • Lindsay J Lynch,
  • Steve B Chukwulebe,
  • Angela M Mexas,
  • Farida Shaheen,
  • Jeffrey N Martin,
  • Steven G Deeks,
  • Mark Connors,
  • Stephen A Migueles,
  • Una O'Doherty

DOI
https://doi.org/10.1371/journal.pone.0071879
Journal volume & issue
Vol. 8, no. 8
p. e71879

Abstract

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Resting CD4+T cells infected with HIV persist in the presence of suppressive anti-viral therapy (ART) and are barriers to a cure. One potential curative approach, therapeutic vaccination, is fueled by recognition of the ability of a subset of elite controllers (EC) to control virus without therapy due to robust anti-HIV immune responses. Controllers have low levels of integrated HIV DNA and low levels of replication competent virus, suggesting a small reservoir. As our recent data indicates some reservoir cells can produce HIV proteins (termed GPR cells for Gag-positive reservoir cells), we hypothesized that a fraction of HIV-expressing resting CD4+T cells could be efficiently targeted and cleared in individuals who control HIV via anti-HIV cytotoxic T lymphocytes (CTL). To test this we examined if superinfected resting CD4+T cells from EC express HIV Gag without producing infectious virus and the susceptibility of these cells to CTL. We found that resting CD4+T cells expressed HIV Gag and were cleared by autologous CD8+T cells from EC. Importantly, we found the extent of CTL clearance in our in vitro assay correlates with in vivo reservoir size and that a population of Gag expressing resting CD4+T cells exists in vivo in patients well controlled on therapy.