IL-21 enhances the cytotoxicity of intratumoral CD8+ T cells, improving radiation efficacy

IL-21增强肿瘤内CD8+ T细胞的细胞毒性,从而提高放射治疗疗效。

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作者:Xin-Yang Li,Xue-Qi Xie,Bao-Chao Wei,Xiao-Zheng Sun,Min-Xin Chen,Ru-Fei Liu,Qing-Xu Tao,Yi-Heng Huang,Qian Wang,Shuang-Shuang Ma,Ling Wei,Rong Xiao,Zhao-Yun Liu,Jin-Ming Yu,Meng Wu,Dawei Chen

Abstract

Radiotherapy is a critical modality in cancer treatment, not only to eradicate cancer cells but also to trigger antitumor immunity. IL-21, an immunomodulatory cytokine with potential in cancer therapy, has unexplored synergy with radiotherapy. Our study, leveraging human cancer databases and tissue microarrays, identified a positive correlation between IL-21 and radiotherapy outcomes, particularly in tumor microenvironment (TME) activation. In mouse tumor models, IL-21 combined with radiation significantly enhanced the TME, boosting CD8+ T cell activation and function, reducing tumor burden, and extending survival. Single-cell transcriptome sequencing revealed that the combination of IL-21 and radiation increased the cytotoxicity of effector and memory CD8+ T cells and prevented their exhaustion. These effects were further validated in humanized mice, where IL-21 combined with radiation reduced A549 tumor growth and enhanced CD8+ T cell function. Post-neoadjuvant radiotherapy samples from patients with esophageal cancer showed a positive correlation between IL-21 levels and CD8+ T cell infiltration. Our findings suggest that IL-21 is a promising adjuvant to radiotherapy, potentially improving treatment efficacy through TME enhancement. This study provides a foundation for future clinical exploration of IL-21 for enhancing radiotherapy.

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