Nature Communications (Nov 2023)

Unlocking the potential of allogeneic Vδ2 T cells for ovarian cancer therapy through CD16 biomarker selection and CAR/IL-15 engineering

  • Derek Lee,
  • Zachary Spencer Dunn,
  • Wenbin Guo,
  • Carl J. Rosenthal,
  • Natalie E. Penn,
  • Yanqi Yu,
  • Kuangyi Zhou,
  • Zhe Li,
  • Feiyang Ma,
  • Miao Li,
  • Tsun-Ching Song,
  • Xinjian Cen,
  • Yan-Ruide Li,
  • Jin J. Zhou,
  • Matteo Pellegrini,
  • Pin Wang,
  • Lili Yang

DOI
https://doi.org/10.1038/s41467-023-42619-2
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 19

Abstract

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Abstract Allogeneic Vγ9Vδ2 (Vδ2) T cells have emerged as attractive candidates for developing cancer therapy due to their established safety in allogeneic contexts and inherent tumor-fighting capabilities. Nonetheless, the limited clinical success of Vδ2 T cell-based treatments may be attributed to donor variability, short-lived persistence, and tumor immune evasion. To address these constraints, we engineer Vδ2 T cells with enhanced attributes. By employing CD16 as a donor selection biomarker, we harness Vδ2 T cells characterized by heightened cytotoxicity and potent antibody-dependent cell-mediated cytotoxicity (ADCC) functionality. RNA sequencing analysis supports the augmented effector potential of Vδ2 T cells derived from CD16 high (CD16Hi) donors. Substantial enhancements are further achieved through CAR and IL-15 engineering methodologies. Preclinical investigations in two ovarian cancer models substantiate the effectiveness and safety of engineered CD16Hi Vδ2 T cells. These cells target tumors through multiple mechanisms, exhibit sustained in vivo persistence, and do not elicit graft-versus-host disease. These findings underscore the promise of engineered CD16Hi Vδ2 T cells as a viable therapeutic option for cancer treatment.