EZH2 identifies the precursors of human natural killer cells with trained immunity

EZH2 identifies the precursors of human natural killer cells with trained immunity

Trained immunity of natural killer (NK) cells has shown great potential in the treatment of cancers by eliciting enhanced effector responses to restimulation by cytokines or cancer cells for long time periods after preactivation. However, the human NK cells responsible for the generation and mainten...

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Veröffentlicht in:Cancer biology & medicine 2021-11, Vol.18 (4), p.1021-1039
Hauptverfasser: Zhang, Chen, Yin, Jie, Zheng, Jian, Xiao, Jun, Hu, Jiajian, Su, Yudong, Zhou, Kaichen, Zhang, Yingchi, Zhang, Xuzhen, Zhang, Hong, Sun, Qian, Wang, Yang, Yu, Wenwen, Wei, Feng, Zhao, Qiang, Li, Long, Ren, Xiubao
Format: Artikel
Sprache:eng
Schlagworte:
CD57 antigen
cell cycle
Cytokines
Epigenetics
ezh2
Flow cytometry
Interleukin 1
Interleukin 12
Interleukin 12 receptors
Interleukin 15
Interleukin 15 receptors
Interleukin 18
Interleukin 18 receptors
Natural killer cells
NKG2 antigen
Original
Phenotypes
precursor
trained immunity
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Zusammenfassung:Trained immunity of natural killer (NK) cells has shown great potential in the treatment of cancers by eliciting enhanced effector responses to restimulation by cytokines or cancer cells for long time periods after preactivation. However, the human NK cells responsible for the generation and maintenance of trained immunity are largely unknown. We hypothesized that heterogeneous human NK cells would respond differentially to stimulation with a combination of IL-12, IL-15, and IL-18, and that an NK cell subset might exist that is mainly responsible for the induction of trained immunity. On the basis of our hypothesis, we aimed to identify the subset from which cytokine-trained human NK cells originate and to explore possible regulatory targets for drug intervention. Flow cytometry assays were performed to analyze the functions of cytokine-trained NK cells and examine cell division and protein expression in NK cell subsets. Single-cell RNA sequencing (scRNA-seq) plus TotalSeq™ technology was used to track the heterogeneity of NK cells during the induction of trained immunity. Traditional developmental markers for peripheral NK cells were unable to identify the precursors of human NK cells with trained immunity. Therefore, we used scRNA-seq plus TotalSeq™ technology to track the heterogeneity of NK cells during the induction of trained immunity and identified a unique cluster of CD57 NKG2A EZH2 IFNG MKI67 IL12R IL15R IL18R NK cells. Enrichment and pseudotime trajectory analyses suggested that this cluster of NK cells contained the precursor of trained NK cells. We then used flow cytometry to further investigate the role of EZH2 in trained NK precursors and found that CD57 NKG2A EZH2 NK cells had faster cell cycles and an enhanced trained phenotype, and EZH2 inhibition significantly impaired the induction of trained immunity in NK cells. These results suggested that EZH2 is a unique epigenetic marker of precursors of human NK cells with trained immunity. Our work revealed human NK heterogeneity in the induction of trained immunity, identified the precursor subset for trained NK cells, and demonstrated the critical role of EZH2 in the induction of trained immunity in human NK cells.
ISSN:2095-3941
DOI:10.20892/j.issn.2095-3941.2020.0791