Journal of Clinical and Translational Science (Apr 2022)

318 Building A Better CAR: Improving CAR-T Trafficking in Cancer Therapy

  • Yeonsun Hong,
  • Hye-Ran Kim,
  • Brandon L. Walling,
  • John Lozada,
  • Andrea M. Amitrano,
  • Cooper J. Sailer,
  • Kihong Lim,
  • Raj Kumar Mongre,
  • Kyun-Do Kim,
  • Tara Capece,
  • Elena B. Lomakina,
  • Nicholas S. Reilly,
  • Richard E. Waugh,
  • Patrick M. Reagan,
  • Minsoo Kim,
  • Patrick W. Oakes,
  • Chang-Duk Jun

DOI
https://doi.org/10.1017/cts.2022.177
Journal volume & issue
Vol. 6
pp. 57 – 57

Abstract

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OBJECTIVES/GOALS: #NAME? METHODS/STUDY POPULATION: Cell culture & protein identification: human T cells were purified from healthy blood, then activated & cultured for 5d. CAR-T cells were collected from infusion bags of cancer patients undergoing CAR-T. Silver staining of naive & activated healthy T-cell lysates was compared; B-II spectrin was upregulated and confirmed by Western blot. Migration assays: naive & activated T-cells were imaged during migration on ICAM-1 and ICAM-1 + CXCL12 coated plates. T-cells were transfected with BII-spectrin cDNA & the chemokine dependence of migration was compared with controls. In-vivo studies: in a melanoma mouse model, BII-spectrin transfected or control T-cells were injected; tumors were followed with serial imaging. Human patient records were examined to correlate endogenous BII-spectrin levels and CAR-T response. RESULTS/ANTICIPATED RESULTS: Activated T-cells downregulate the cytoskeletal protein B-II spectrin compared to naive cells, leading to chemokine-independent migration in in vitro assays and off-target trafficking when CAR-T cells are given in vivo. Restoration of B-II spectrin levels via transfection restores chemokine-dependence of activated T-cells. In a mouse melanoma model, control mice injected with standard activated T-cells showed fewer cells in the tumor site and more cells in the off-target organs (spleen, lungs) when compared to mice injected with B-II spectrin transfected cells. Furthermore, among 3 human patients undergoing CAR-T therapy, those with higher endogenous B-II spectrin levels experienced fewer side-effects, measured by the neurotoxicity and cytokine release syndrome grades. DISCUSSION/SIGNIFICANCE: A major hurdle to widespread CAR-T therapy for cancer is significant, often fatal side-effects. Our work shows that the protein B-II spectrin is downregulated during CAR-T production, and that restoring B-II spectrin levels decreases side-effects while increasing tumor clearance--hopefully translating to better CAR-T regimens for the future.