Single-cell sequencing reveals immune features of treatment response to neoadjuvant immunochemotherapy in esophageal squamous cell carcinoma

被引:0
|
作者
Zhenlin Yang [1 ]
He Tian [1 ]
Xiaowei Chen [2 ]
Bozhao Li [1 ]
Guangyu Bai [3 ]
Qingyuan Cai [1 ]
Jiachen Xu [4 ]
Wei Guo [5 ]
Shuaibo Wang [6 ]
Yue Peng [1 ]
Qing Liang [1 ]
Liyan Xue [7 ]
Shugeng Gao [1 ]
机构
[1] Chinese Academy of Medical Sciences and Peking Union Medical College,Department of Thoracic Surgery, National Cancer Center/National Clinical Research Center for Cancer/Cancer Hospital
[2] Chinese Academy of Medical Sciences and Peking Union Medical College,Department of Respiratory Medicine, Fuwai Hospital, National Center for Cardiovascular Diseases
[3] National Center for Nanoscience and Technology,CAS Key Laboratory for Biomedical Effects of Nanomaterials and Nanosafety, CAS Center for Excellence in Nanoscience
[4] Peking University,BIOPIC, Peking
[5] Chinese Academy of Medical Sciences and Peking Union Medical College,Tsinghua Center for Life Sciences, Academy for Advanced Interdisciplinary Studies, School of Life Sciences, International Cancer Institute
[6] Guangdong Provincial Key Lab of Translational Medicine in Lung Cancer,Department of Medical Oncology, National Cancer Center/ National Clinical Research Center for Cancer/Cancer Hospital
[7] Capital Medical University,Guangdong Provincial People’s Hospital/Guangdong Provincial Academy of Medical Sciences
[8] Chinese Academy of Medical Sciences and Peking Union Medical College,Department of Thoracic Surgery, Beijing Chao
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D O I
10.1038/s41467-024-52977-0
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摘要
Neoadjuvant immunochemotherapy (nICT) has dramatically changed the treatment landscape of operable esophageal squamous cell carcinoma (ESCC), but factors influencing tumor response to nICT are not well understood. Here, using single-cell RNA sequencing paired with T cell receptor sequencing, we profile tissues from ESCC patients accepting nICT treatment and characterize the tumor microenvironment context. CXCL13+CD8+ Tex cells, a subset of exhausted CD8+ T cells, are revealed to highly infiltrate in pre-treatment tumors and show prominent progenitor exhaustion phenotype in post-treatment samples from responders. We validate CXCL13+CD8+ Tex cells as a predictor of improved response to nICT and reveal CXCL13 to potentiate anti-PD-1 efficacy in vivo. Post-treatment tumors from non-responders are enriched for CXCL13+CD8+ Tex cells with notably remarkable exhaustion phenotype and TNFRSF4+CD4+ Tregs with activated immunosuppressive function and a significant clone expansion. Several critical markers for therapeutic resistance are also identified, including LRRC15+ fibroblasts and SPP1+ macrophages, which may recruit Tregs to form an immunosuppressive landscape. Overall, our findings unravel immune features of distinct therapeutic response to nICT treatment, providing a rationale for optimizing individualized neoadjuvant strategy in ESCC.
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