Frontiers in Immunology (Jan 2019)

Antigen Production After Latency Reversal and Expression of Inhibitory Receptors in CD8+ T Cells Limit the Killing of HIV-1 Reactivated Cells

  • Alba Ruiz,
  • Alba Ruiz,
  • Oscar Blanch-Lombarte,
  • Oscar Blanch-Lombarte,
  • Esther Jimenez-Moyano,
  • Dan Ouchi,
  • Beatriz Mothe,
  • Beatriz Mothe,
  • Ruth Peña,
  • Cristina Galvez,
  • Cristina Galvez,
  • Meritxell Genescà,
  • Javier Martinez-Picado,
  • Javier Martinez-Picado,
  • Javier Martinez-Picado,
  • Philip Goulder,
  • Richard Barnard,
  • Bonnie Howell,
  • Bonaventura Clotet,
  • Bonaventura Clotet,
  • Julia G. Prado,
  • Julia G. Prado

DOI
https://doi.org/10.3389/fimmu.2018.03162
Journal volume & issue
Vol. 9

Abstract

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The so-called shock and kill therapies aim to combine HIV-1 reactivation by latency-reversing agents (LRA) with immune clearance to purge the HIV-1 reservoir. The clinical use of LRA has demonstrated detectable perturbations in the HIV-1 reservoir without measurable reductions to date. Consequently, fundamental questions concerning the limitations of the recognition and killing of LRA-reactivated cells by effector cells such as CD8+ T cells remain to be answered. Here, we developed a novel experimental framework where we combine the use of cytotoxic CD8+ T-cell lines and ex vivo CD8+ T cells from HIV-1-infected individuals with functional assays of LRA-inducible reactivation to delineate immune barriers to clear the reservoir. Our results demonstrate the potential for early recognition and killing of reactivated cells by CD8+ T cells. However, the potency of LRAs when crossing the barrier for antigen presentation in target cells, together with the lack of expression of inhibitory receptors in CD8+ T cells, are critical events to maximize the speed of recognition and the magnitude of the killing of LRA-inducible provirus. Taken together, our findings highlight direct limitations in LRA potency and CD8+ T cell functional status to succeed in the cure of HIV-1 infection.

Keywords