CAR-T Cells with Phytohemagglutinin (PHA) Provide Anti-Cancer Capacity with Better Proliferation, Rejuvenated Effector Memory, and Reduced Exhausted T Cell Frequencies

Gamze Gulden; Berranur Sert; Tarik Teymur; Yasin Ay; Nulifer Neslihan Tiryaki; Abhinava K Mishra; Ercument Ovali; Nevzat Tarhan; Cihan Tastan

doi:10.3390/vaccines11020313

CAR-T Cells with Phytohemagglutinin (PHA) Provide Anti-Cancer Capacity with Better Proliferation, Rejuvenated Effector Memory, and Reduced Exhausted T Cell Frequencies

Vaccines (Basel). 2023 Jan 31;11(2):313. doi: 10.3390/vaccines11020313.

Authors

Gamze Gulden^{1

2}, Berranur Sert^{1

2}, Tarik Teymur^{2

3}, Yasin Ay^{1

2}, Nulifer Neslihan Tiryaki^{2

3}, Abhinava K Mishra⁴, Ercument Ovali⁵, Nevzat Tarhan⁶, Cihan Tastan^{2

3}

Affiliations

¹ Molecular Biology, Institute of Science and Technology, Üsküdar University, Istanbul 34662, Turkey.
² Transgenic Cell Technologies and Epigenetic Application and Research Center (TRGENMER), Üsküdar University, Istanbul 34662, Turkey.
³ Molecular Biology and Genetics Department, Faculty of Engineering and Natural Science, Üsküdar University, Istanbul 34662, Turkey.
⁴ Molecular, Cellular and Developmental Biology Department, University of California Santa Barbara, Santa Barbara, CA 93106, USA.
⁵ Acıbadem Labcell Cellular Therapy Laboratory, Istanbul 34752, Turkey.
⁶ Faculty of Humanities and Social Sciences, Üsküdar University, Istanbul 34662, Turkey.

Abstract

The development of genetic modification techniques has led to a new era in cancer treatments that have been limited to conventional treatments such as chemotherapy. intensive efforts are being performed to develop cancer-targeted therapies to avoid the elimination of non-cancerous cells. One of the most promising approaches is genetically modified CAR-T cell therapy. The high central memory T cell (Tcm) and stem cell-like memory T cell (Tscm) ratios in the CAR-T cell population increase the effectiveness of immunotherapy. Therefore, it is important to increase the populations of CAR-expressing Tcm and Tscm cells to ensure that CAR-T cells remain long-term and have cytotoxic (anti-tumor) efficacy. In this study, we aimed to improve CAR-T cell therapy's time-dependent efficacy and stability, increasing the survival time and reducing the probability of cancer cell growth. To increase the sub-population of Tcm and Tscm in CAR-T cells, we investigated the production of a long-term stable and efficient cytotoxic CAR-T cell by modifications in the cell activation-dependent production using Phytohemagglutinin (PHA). PHA, a lectin that binds to the membranes of T cells and increases metabolic activity and cell division, is studied to increase the Tcm and Tscm population. Although it is known that PHA significantly increases Tcm cells, B-lymphocyte antigen CD19-specific CAR-T cell expansion, its anti-cancer and memory capacity has not yet been tested compared with aCD3/aCD28-amplified CAR-T cells. Two different types of CARs (aCD19 scFv CD8-(CD28 or 4-1BB)-CD3z-EGFRt)-expressing T cells were generated and their immunogenic phenotype, exhausted phenotype, Tcm-Tscm populations, and cytotoxic activities were determined in this study. The proportion of T cell memory phenotype in the CAR-T cell populations generated by PHA was observed to be higher than that of aCD3/aCD28-amplified CAR-T cells with similar and higher proliferation capacity. Here, we show that PHA provides long-term and efficient CAR-T cell production, suggesting a potential alternative to aCD3/aCD28-amplified CAR-T cells.

Keywords: CAR-T; immunologic memory; immunotherapy; leukemia; phytohemagglutinin.

Grants and funding

4293/The Presidency of Turkish Health Institutes (TUSEB)