Patient‐derived Immunocompetent Tumor Organoids: A Platform for Chemotherapy Evaluation in the Context of T‐cell Recognition

Patient‐derived Immunocompetent Tumor Organoids: A Platform for Chemotherapy Evaluation in the Context of T‐cell Recognition

Most of the anticancer compounds synthesized by chemists are primarily evaluated for their direct cytotoxic effects at the cellular level, often overlooking the critical role of the immune system. In this study, we developed a patient‐derived, T‐cell‐retaining tumor organoid model that allows us to...

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Veröffentlicht in:Angewandte Chemie 2024-02, Vol.136 (9), p.n/a
Hauptverfasser: Zhao, Zihan, Zhang, Shuren, Jiang, Ning, Zhu, Wenjie, Song, Dongfan, Liu, Siyang, Yu, Wenhao, Bai, Yuhao, Zhang, Yulin, Wang, Xiaoyu, Zhong, Xuanmeng, Guo, Hongqian, Guo, Zijian, Yang, Rong, Li, Jie P.
Format: Artikel
Sprache:eng
Schlagworte:
Anticancer properties
Bladder Cancer
Cancer
Cell recognition
Chemotherapy
Cytotoxicity
Drugs
Immune checkpoint inhibitors
Immune system
Immunocompetence
Immunocompetent Tumor Organoid
Immunosuppressive agents
Lymphocytes
Lymphocytes T
Metalloimmunology
Organoids
Synergistic effect
T cell receptors
T-Cell Recognition
Tumors
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Zusammenfassung:Most of the anticancer compounds synthesized by chemists are primarily evaluated for their direct cytotoxic effects at the cellular level, often overlooking the critical role of the immune system. In this study, we developed a patient‐derived, T‐cell‐retaining tumor organoid model that allows us to evaluate the anticancer efficacy of chemical drugs under the synergistic paradigm of antigen‐specific T‐cell‐dependent killing, which may reveal the missed drug hits in the simple cytotoxic assay. We evaluated clinically approved platinum (Pt) drugs and a custom library of twenty‐eight PtIV compounds. We observed low direct cytotoxicity of Pt drugs, but variable synergistic effects in combination with immune checkpoint inhibitors (ICIs). In contrast, the majority of PtIV compounds exhibited potent tumor‐killing capabilities. Interestingly, several PtIV compounds went beyond direct tumor killing and showed significant immunosynergistic effects with ICIs, outstanding at sub‐micromolar concentrations. Among these, Pt‐19, PtIV compounds with cinnamate axial ligands, emerged as the most therapeutically potent, demonstrating pronounced immunosynergistic effects by promoting the release of cytotoxic cytokines, activating immune‐related pathways and enhancing T cell receptor (TCR) clonal expansion. Overall, this initiative marks the first use of patient‐derived immunocompetent tumor organoids to explore and study chemotherapy, advancing their path toward more effective small molecule drug discovery. A patient‐derived, T‐cell‐retaining tumor organoid model to rapidly, precisely and individually evaluate the anticancer efficacy of chemical drugs under the synergistic paradigm of antigen‐specific T‐cell‐dependent killing is presented. This study bridges the gap between clinical translation and basic research in metalloimmunology, accelerating drug discovery for cancer immunotherapy and facilitating individualized precision medicine.
ISSN:0044-8249
1521-3757
DOI:10.1002/ange.202317613