JCI Insight (Jan 2021)

Stem cell–derived CAR T cells traffic to HIV reservoirs in macaques

  • Isaac M. Barber-Axthelm,
  • Valerie Barber-Axthelm,
  • Kai Yin Sze,
  • Anjie Zhen,
  • Gajendra W. Suryawanshi,
  • Irvin S.Y. Chen,
  • Jerome A. Zack,
  • Scott G. Kitchen,
  • Hans-Peter Kiem,
  • Christopher W. Peterson

Journal volume & issue
Vol. 6, no. 1

Abstract

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Allogeneic hematopoietic stem cell transplantation (allo-HSCT) with CCR5– donor cells is the only treatment known to cure HIV-1 in patients with underlying malignancy. This is likely due to a donor cell–mediated graft-versus-host effect targeting HIV reservoirs. Allo-HSCT would not be an acceptable therapy for most people living with HIV due to the transplant-related side effects. Chimeric antigen receptor (CAR) immunotherapies specifically traffic to malignant lymphoid tissues (lymphomas) and, in some settings, are able to replace allo-HSCT. Here, we quantified the engraftment of HSC-derived, virus-directed CAR T cells within HIV reservoirs in a macaque model of HIV infection, using potentially novel IHC assays. HSC-derived CAR cells trafficked to and displayed multilineage engraftment within tissue-associated viral reservoirs, persisting for nearly 2 years in lymphoid germinal centers, the brain, and the gastrointestinal tract. Our findings demonstrate that HSC-derived CAR+ cells reside long-term and proliferate in numerous tissues relevant for HIV infection and cancer.

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