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CD39hi identifies an exhausted tumor-reactive CD8+ T cell population associated with tumor progression in human gastric cancer

Authors :
Yang Shen
Yuan Qiu
Zhen-quan Duan
Yu-xian Li
Ying Wang
Yuan-yuan Zhang
Bao-hang Zhu
Xiao-hong Yu
Xue-ling Tan
Weisan Chen
Yuan Zhuang
Quan-ming Zou
Dai-yuan Ma
Liu-sheng Peng
Source :
Pharmacological Research, Vol 202, Iss , Pp 107122- (2024)
Publication Year :
2024
Publisher :
Elsevier, 2024.

Abstract

The ectonucleotidase CD39 has been regarded as a promising immune checkpoint in solid tumors. However, the expression of CD39 by tumor-infiltrating CD8+ T cells as well as their potential roles and clinical implications in human gastric cancer (GC) remain largely unknown. Here, we found that GC-infiltrating CD8+ T cells contained a fraction of CD39hi cells that constituted about 6.6% of total CD8+ T cells in tumors. These CD39hi cells enriched for GC-infiltrating CD8+ T cells with features of exhaustion in transcriptional, phenotypic, metabolic and functional profiles. Additionally, GC-infiltrating CD39hiCD8+ T cells were also identified for tumor-reactive T cells, as these cells expanded in vitro were able to recognize autologous tumor organoids and induced more tumor cell apoptosis than those of expanded their CD39int and CD39-CD8+ counterparts. Furthermore, CD39 enzymatic activity controlled GC-infiltrating CD39hiCD8+ T cell effector function, and blockade of CD39 efficiently enhanced their production of cytokines IFN-γ and TNF-α. Finally, high percentages of GC-infiltrating CD39hiCD8+ T cells correlated with tumor progression and independently predicted patients’ poor overall survival. These findings provide novel insights into the association of CD39 expression level on CD8+ T cells with their features and potential clinical implications in GC, and empowering those exhausted tumor-reactive CD39hiCD8+ T cells through CD39 inhibition to circumvent the suppressor program may be an attractive therapeutic strategy against GC.

Details

Language :
English
ISSN :
10961186
Volume :
202
Issue :
107122-
Database :
Directory of Open Access Journals
Journal :
Pharmacological Research
Publication Type :
Academic Journal
Accession number :
edsdoj.70c96084701b405bbfeb2784adbe514e
Document Type :
article
Full Text :
https://doi.org/10.1016/j.phrs.2024.107122