Scientific Reports (Sep 2024)

Engineering potent chimeric antigen receptor T cells by programming signaling during T-cell activation

  • Aileen W. Li,
  • Jessica D. Briones,
  • Jia Lu,
  • Quinn Walker,
  • Rowena Martinez,
  • Hajime Hiraragi,
  • Bijan A. Boldajipour,
  • Purnima Sundar,
  • Shobha Potluri,
  • Gary Lee,
  • Omar A. Ali,
  • Alexander S. Cheung

DOI
https://doi.org/10.1038/s41598-024-72392-1
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 14

Abstract

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Abstract Programming cell signaling during T-cell activation represents a simple strategy for improving the potency of therapeutic T-cell products. Stim-R technology (Lyell Immunopharma) is a customizable, degradable synthetic cell biomimetic that emulates physiologic, cell-like presentation of signal molecules to control T-cell activation. A breadth of Stim-R formulations with different anti-CD3/anti-CD28 (αCD3/αCD28) antibody densities and stoichiometries were screened for their effects on multiple metrics of T-cell function. We identified an optimized formulation that produced receptor tyrosine kinase-like orphan receptor 1 (ROR1)-targeted chimeric antigen receptor (CAR) T cells with enhanced persistence and polyfunctionality in vitro, as assessed in repeat-stimulation assays, compared with a benchmark product generated using a conventional T-cell–activating reagent. In transcriptomic analyses, CAR T cells activated with Stim-R technology showed downregulation of exhaustion-associated gene sets and retained a unique subset of stem-like cells with effector-associated gene signatures following repeated exposure to tumor cells. Compared with the benchmark product, CAR T cells activated using the optimized Stim-R technology formulation exhibited higher peak expansion, prolonged persistence, and improved tumor control in a solid tumor xenograft model. Enhancing T-cell products with Stim-R technology during T-cell activation may help improve therapeutic efficacy against solid tumors.