Global characterization of T cells in non-small-cell lung cancer by single-cell sequencing

肺癌 CD8型 腺癌 生物 细胞毒性T细胞 T细胞 癌症研究 单细胞测序 癌症 抗原 细胞 免疫学 医学 免疫系统 基因 病理 内科学 表型 外显子组测序 遗传学 体外
作者
Xinyi Guo,Yuanyuan Zhang,Liangtao Zheng,Chunhong Zheng,Jintao Song,Qiming Zhang,Boxi Kang,Zhouzerui Liu,Lina Jin,Rui Xing,Ranran Gao,Lei Zhang,Min Dong,Xueda Hu,Xianwen Ren,Dennis Kirchhoff,Helge G. Roider,Tao Yan,Zemin Zhang
出处
期刊:Nature Medicine [Springer Nature]
卷期号:24 (7): 978-985 被引量:1015
标识
DOI:10.1038/s41591-018-0045-3
摘要

Cancer immunotherapies have shown sustained clinical responses in treating non-small-cell lung cancer1-3, but efficacy varies and depends in part on the amount and properties of tumor infiltrating lymphocytes4-6. To depict the baseline landscape of the composition, lineage and functional states of tumor infiltrating lymphocytes, here we performed deep single-cell RNA sequencing for 12,346 T cells from 14 treatment-naïve non-small-cell lung cancer patients. Combined expression and T cell antigen receptor based lineage tracking revealed a significant proportion of inter-tissue effector T cells with a highly migratory nature. As well as tumor-infiltrating CD8+ T cells undergoing exhaustion, we observed two clusters of cells exhibiting states preceding exhaustion, and a high ratio of "pre-exhausted" to exhausted T cells was associated with better prognosis of lung adenocarcinoma. Additionally, we observed further heterogeneity within the tumor regulatory T cells (Tregs), characterized by the bimodal distribution of TNFRSF9, an activation marker for antigen-specific Tregs. The gene signature of those activated tumor Tregs, which included IL1R2, correlated with poor prognosis in lung adenocarcinoma. Our study provides a new approach for patient stratification and will help further understand the functional states and dynamics of T cells in lung cancer.
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