PLoS Pathogens (Mar 2020)

The human IL-15 superagonist N-803 promotes migration of virus-specific CD8+ T and NK cells to B cell follicles but does not reverse latency in ART-suppressed, SHIV-infected macaques.

  • Gabriela M Webb,
  • Jhomary Molden,
  • Kathleen Busman-Sahay,
  • Shaheed Abdulhaqq,
  • Helen L Wu,
  • Whitney C Weber,
  • Katherine B Bateman,
  • Jason S Reed,
  • Mina Northrup,
  • Nicholas Maier,
  • Shiho Tanaka,
  • Lina Gao,
  • Brianna Davey,
  • Benjamin L Carpenter,
  • Michael K Axthelm,
  • Jeffrey J Stanton,
  • Jeremy Smedley,
  • Justin M Greene,
  • Jeffrey T Safrit,
  • Jacob D Estes,
  • Pamela J Skinner,
  • Jonah B Sacha

DOI
https://doi.org/10.1371/journal.ppat.1008339
Journal volume & issue
Vol. 16, no. 3
p. e1008339

Abstract

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Despite the success of antiretroviral therapy (ART) to halt viral replication and slow disease progression, this treatment is not curative and there remains an urgent need to develop approaches to clear the latent HIV reservoir. The human IL-15 superagonist N-803 (formerly ALT-803) is a promising anti-cancer biologic with potent immunostimulatory properties that has been extended into the field of HIV as a potential "shock and kill" therapeutic for HIV cure. However, the ability of N-803 to reactivate latent virus and modulate anti-viral immunity in vivo under the cover of ART remains undefined. Here, we show that in ART-suppressed, simian-human immunodeficiency virus (SHIV)SF162P3-infected rhesus macaques, subcutaneous administration of N-803 activates and mobilizes both NK cells and SHIV-specific CD8+ T cells from the peripheral blood to lymph node B cell follicles, a sanctuary site for latent virus that normally excludes such effector cells. We observed minimal activation of memory CD4+ T cells and no increase in viral RNA content in lymph node resident CD4+ T cells post N-803 administration. Accordingly, we found no difference in the number or magnitude of plasma viremia timepoints between treated and untreated animals during the N-803 administration period, and no difference in the size of the viral DNA cell-associated reservoir post N-803 treatment. These results substantiate N-803 as a potent immunotherapeutic candidate capable of activating and directing effector CD8+ T and NK cells to the B cell follicle during full ART suppression, and suggest N-803 must be paired with a bona fide latency reversing agent in vivo to facilitate immune-mediated modulation of the latent viral reservoir.