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Enhanced adaptive immune responses in lung adenocarcinoma through natural killer cell stimulation.


ABSTRACT: Natural killer (NK) cells inhibit tumor development in mouse models and their presence in tumors correlates with patient survival. However, tumor-associated NK cells become dysfunctional; thus, stimulation of NK cells in cancer is emerging as an attractive immunotherapeutic strategy. In a mouse model of lung adenocarcinoma, NK cells localized to tumor stroma with immature phenotypes and low functional capacity. To test their responsiveness within established disease, we engineered a system for inducible expression of activating ligands in tumors. After stimulation, NK cells localized inside tumors, with increased cytokine production capacity. Strikingly, T cells were also recruited to tumors in an NK cell-dependent manner, and exhibited higher functionality. In neoantigen-expressing tumors, NK cell stimulation enhanced the number and function of tumor-specific T cells and, in long-term settings, reduced tumor growth. Thus, even in established disease NK cells can be activated to contribute to antitumor immunity, supporting their potential as an important target in cancer immunotherapy.

SUBMITTER: Schmidt L 

PROVIDER: S-EPMC6717259 | biostudies-literature | 2019 Aug

REPOSITORIES: biostudies-literature

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Enhanced adaptive immune responses in lung adenocarcinoma through natural killer cell stimulation.

Schmidt Leah L   Eskiocak Banu B   Kohn Ryan R   Dang Celeste C   Joshi Nikhil S NS   DuPage Michel M   Lee Da-Yae DY   Jacks Tyler T  

Proceedings of the National Academy of Sciences of the United States of America 20190813 35


Natural killer (NK) cells inhibit tumor development in mouse models and their presence in tumors correlates with patient survival. However, tumor-associated NK cells become dysfunctional; thus, stimulation of NK cells in cancer is emerging as an attractive immunotherapeutic strategy. In a mouse model of lung adenocarcinoma, NK cells localized to tumor stroma with immature phenotypes and low functional capacity. To test their responsiveness within established disease, we engineered a system for i  ...[more]

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