Single-cell profiling reveals distinct immune response landscapes in tuberculous pleural effusion and non-TPE

免疫系统 医学 胸腔积液 免疫学 肺结核 结核分枝杆菌 人口 病理 癌症研究 内科学 环境卫生
作者
Xinting Yang,Jun Yan,Yu Xue,Qing Sun,Yun Zhang,Guo Ru,Chao-hong Wang,Xuelian Li,Qingtao Liang,Hangyu Wu,Chong Wang,Xinlei Liao,Sibo Long,Maike Zheng,Rongrong Wei,Haoran Zhang,Yi Liu,Nanying Che,Laurence Don Wai Luu,Junhua Pan,Guirong Wang,Yi Wang
出处
期刊:Frontiers in Immunology [Frontiers Media]
卷期号:14 被引量:10
标识
DOI:10.3389/fimmu.2023.1191357
摘要

Background Tuberculosis (TB) is caused by Mycobacterium tuberculosis ( Mtb ) and remains a major health threat worldwide. However, a detailed understanding of the immune cells and inflammatory mediators in Mtb -infected tissues is still lacking. Tuberculous pleural effusion (TPE), which is characterized by an influx of immune cells to the pleural space, is thus a suitable platform for dissecting complex tissue responses to Mtb infection. Methods We employed singe-cell RNA sequencing to 10 pleural fluid (PF) samples from 6 patients with TPE and 4 non-TPEs including 2 samples from patients with TSPE (transudative pleural effusion) and 2 samples with MPE (malignant pleural effusion). Result Compared to TSPE and MPE, TPE displayed obvious difference in the abundance of major cell types (e.g., NK, CD4+T, Macrophages), which showed notable associations with disease type. Further analyses revealed that the CD4 lymphocyte population in TPE favored a Th1 and Th17 response. Tumor necrosis factors (TNF)-, and XIAP related factor 1 (XAF1)-pathways induced T cell apoptosis in patients with TPE. Immune exhaustion in NK cells was an important feature in TPE. Myeloid cells in TPE displayed stronger functional capacity for phagocytosis, antigen presentation and IFN-γ response, than TSPE and MPE. Systemic elevation of inflammatory response genes and pro-inflammatory cytokines were mainly driven by macrophages in patients with TPE. Conclusion We provide a tissue immune landscape of PF immune cells, and revealed a distinct local immune response in TPE and non-TPE (TSPE and MPE). These findings will improve our understanding of local TB immunopathogenesis and provide potential targets for TB therapy.

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