Natural and revolutionary tumor-specific T-cell therapy
Zhi Dai, Xue-Meng Liu, Yun-li Zhao, Li-Xing Zhao, Xiao-Dong Luo

TL;DR
A new T-cell therapy was developed that avoids viruses and professional antigen-presenting cells, showing promise in targeting tumors without causing secondary cancers.
Contribution
A novel tumor-specific T-cell therapy was developed without using lentivirus or professional APCs, enabling safer and more specific cancer treatment.
Findings
Tumor-specific T-cells were generated by co-culturing MHC+ cancer cells and naïve T-cells with CD28 signals.
The therapy reduced tumor nodules by 90% and improved survival in mice.
Tumor-specific T-cells could be easily separated and produced from peripheral blood.
Abstract
Recently the FDA conducted a risk investigation and labeled the Boxed Warning for all BCMA- and CD19-directed CAR-T cell therapy, so does it mean that the public must take risk of secondary cancer to receive cell therapy? Here, without lentivirus and professional antigen presenting cell application, a novel tumor-specific T-cell therapy was successfully developed only by co-culturing MHC+ cancer cells and Naïve-T cells under the CD28 co-stimulatory signals. These tumor-specific T-cells could be separated through cell size and abundantly produced from peripheral blood, and would spontaneously attack target cells that carrying the same tumor antigen while avoiding others in vitro test. Moreover, it markedly decreased 90% tumor nodules companying with greatly improving overall survival (76 days vs 30 days) after twice infusion back to mice. This work maximally avoided the risks of…
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Taxonomy
TopicsCAR-T cell therapy research · Virus-based gene therapy research · Immunotherapy and Immune Responses
