Tumor buster - where will the CAR-T cell therapy ‘missile’ go?

Author:

Qu Chunrun,Zhang Hao,Cao Hui,Tang Lanhua,Mo Haoyang,Liu Fangkun,Zhang Liyang,Yi Zhenjie,Long Lifu,Yan Luzhe,Wang Zeyu,Zhang Nan,Luo Peng,Zhang Jian,Liu Zaoqu,Ye Weijie,Liu Zhixiong,Cheng QuanORCID

Abstract

AbstractChimeric antigen receptor (CAR) T cell (CAR-T cell) therapy based on gene editing technology represents a significant breakthrough in personalized immunotherapy for human cancer. This strategy uses genetic modification to enable T cells to target tumor-specific antigens, attack specific cancer cells, and bypass tumor cell apoptosis avoidance mechanisms to some extent. This method has been extensively used to treat hematologic diseases, but the therapeutic effect in solid tumors is not ideal. Tumor antigen escape, treatment-related toxicity, and the immunosuppressive tumor microenvironment (TME) limit their use of it. Target selection is the most critical aspect in determining the prognosis of patients receiving this treatment. This review provides a comprehensive summary of all therapeutic targets used in the clinic or shown promising potential. We summarize CAR-T cell therapies’ clinical trials, applications, research frontiers, and limitations in treating different cancers. We also explore coping strategies when encountering sub-optimal tumor-associated antigens (TAA) or TAA loss. Moreover, the importance of CAR-T cell therapy in cancer immunotherapy is emphasized.

Publisher

Springer Science and Business Media LLC

Subject

Cancer Research,Oncology,Molecular Medicine

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