Distinct Inflammatory Cytotoxic T Lymphocyte Populations Mediate PD-1 Blockade Induced Immune-Related Adverse Events in Multiple Organs

  • Cancer Res. 2026 May 15. doi: 10.1158/0008-5472.CAN-25-2892.
Xiaowei Liu  1 Jinen Song  1 Fengli Zuo  1 Qian Xiao  1 Jing Yu  1 Huiling Wang  1 Meiling Yuan  1 Leyi Tang  2 Xueyan Wang  1 Xinmin Wang  1 Xiujing He  3 Huifang Li  1 Jing Zhou  1 Jianping Hu  4 Guang Yang  2 Jie Zhang  2 Xiaofei Deng  5 Xuelei Ma  3 Jing Jing  2 Hubing Shi  1
Affiliations
  • 1. West China Hospital of Sichuan University Chengdu, Sichuan China.
  • 2. West China Hospital of Sichuan University China.
  • 3. West China Hospital of Sichuan University Chengdu China.
  • 4. Chengdu University Chengdu, Sichuan China.
  • 5. Yingshan County People's HospitaYingshan County People's Hospita Nanchong China.
Abstract

Immune checkpoint blockade-induced immune-related adverse events (irAEs) hamper the application of this revolutionary anti-tumor therapeutic strategy. Here, we explored the mechanisms driving irAEs by profiling the immune ecosystem of major irAE-affected organs at the single-cell scale. The analysis identified three populations of cytotoxic T lymphocytes that mediate anti-tumor immunity (CTL1) or that induce irAE in the gut (CTLirAE-I) or in multiple Other organs (CTLirAE-II). Interleukin-JAK1 signaling was specifically activated in the CTLirAE-II population upon PD-1 blockade. Targeting JAK1 remarkably relieved the irAEs in the heart and lung, without compromising the anti-tumor efficacy. Tracking TCR sequence and transcriptome showed that CTLirAE-II and CTL1 populations originated from lymph node progenitor cells, while the CTLirAE-I population was derived from tissue-resident memory T cells. Moreover, irAEs could be monitored by assessing the CTLirAE-II population in circulation. In conclusion, this study elucidates the landscape of cellular changes in irAEs across multiple organs following immunotherapy and proposes strategies for relieving irAE symptoms and facilitating diagnosis.

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