Efficient killing of tumor cells by CAR-T cells requires greater number of engaged CARs than TCRs |
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| Authors: | Nadia Anikeeva Sergey Panteleev Nicholas W. Mazzanti Mizue Terai Takami Sato Yuri Sykulev |
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| Affiliation: | 1.Department of Microbiology and Immunology, Thomas Jefferson University, Philadelphia, Pennsylvania, USA;2.Department of Medical Oncology, Thomas Jefferson University, Philadelphia, Pennsylvania, USA;3.Sidney Kimmel Cancer Center, Thomas Jefferson University, Philadelphia, Pennsylvania, USA |
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| Abstract: | Although CAR-T cells are widely used to treat cancer, efficiency of CAR-T cell cytolytic responses has not been carefully examined. We engineered CAR specific for HMW-MAA (high-molecular-weight melanoma-associated antigen) and evaluated potency of CD8+ CAR-T cells to release cytolytic granules and to kill tissue-derived melanoma cells, which express different levels of HMW-MAA. CAR-T cells efficiently killed melanoma cells expressing high level of HMW-MAA, but not melanoma cells with lower levels of HMW-MAA. The same melanoma cells presenting significantly lower level of stimulatory peptide-MHC ligand were readily lysed by T cells transduced with genes encoding α,β-TCR specific for the peptide-MHC ligand. The data suggest that higher level of targeted molecules is required to engage a larger number of CARs than TCRs to induce efficient cytolytic granule release and destruction of melanoma cells. Understanding the difference in molecular mechanisms controlling activation thresholds of CAR- versus TCR-mediated responses will contribute to improving efficiency of CAR T cells required to eliminate solid tumors presenting low levels of targeted molecules. |
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| Keywords: | T-cell receptor (TCR) T-cell bioengineering chimeric antigen receptor (CAR) receptor regulation immunotherapy tumor immunology killing efficiency of various melanoma cells by CAR- or TCR-triggered T-cells |
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