Gene editing technology to improve antitumor T-cell functions in adoptive immunotherapy

被引:0
作者
Yusuke Ito
Satoshi Inoue
Yuki Kagoya
机构
[1] Keio University School of Medicine,Division of Tumor Immunology, Institute for Advanced Medical Research
来源
Inflammation and Regeneration | / 44卷
关键词
Adoptive immunotherapy; Chimeric antigen receptor; Epigenetics; DNA methylation; PRDM1; Memory T cell; T-cell exhaustion; CRISPR/Cas9;
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摘要
Adoptive immunotherapy, in which tumor-reactive T cells are prepared in vitro for adoptive transfer to the patient, can induce an objective clinical response in specific types of cancer. In particular, chimeric antigen receptor (CAR)-redirected T-cell therapy has shown robust responses in hematologic malignancies. However, its efficacy against most of the other tumors is still insufficient, which remains an unmet medical need. Accumulating evidence suggests that modifying specific genes can enhance antitumor T-cell properties. Epigenetic factors have been particularly implicated in the remodeling of T-cell functions, including changes to dysfunctional states such as terminal differentiation and exhaustion. Genetic ablation of key epigenetic molecules prevents the dysfunctional reprogramming of T cells and preserves their functional properties.
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