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CIS is a potent checkpoint in NK cell–mediated tumor immunity

Abstract:
The detection of aberrant cells by natural killer (NK) cells is controlled by the integration of signals from activating and inhibitory ligands and from cytokines such as IL-15. We identified cytokine-inducible SH2-containing protein (CIS, encoded by Cish) as a critical negative regulator of IL-15 signaling in NK cells. Cish was rapidly induced in response to IL-15, and deletion of Cish rendered NK cells hypersensitive to IL-15, as evidenced by enhanced proliferation, survival, IFN-γ production and cytotoxicity toward tumors. This was associated with increased JAK-STAT signaling in NK cells in which Cish was deleted. Correspondingly, CIS interacted with the tyrosine kinase JAK1, inhibiting its enzymatic activity and targeting JAK for proteasomal degradation. Cish−/− mice were resistant to melanoma, prostate and breast cancer metastasis in vivo, and this was intrinsic to NK cell activity. Our data uncover a potent intracellular checkpoint in NK cell–mediated tumor immunity and suggest possibilities for new cancer immunotherapies directed at blocking CIS function.
Publication status:
Published
Peer review status:
Peer reviewed

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Publisher copy:
10.1038/ni.3470

Authors



Publisher:
Springer Nature
Journal:
Nature Immunology More from this journal
Volume:
17
Issue:
7
Pages:
816-824
Publication date:
2016-05-23
Acceptance date:
2016-04-27
DOI:
EISSN:
1529-2916
ISSN:
1529-2908


Language:
English
Keywords:
Pubs id:
pubs:625356
UUID:
uuid:a2dd7142-2d7e-45a3-8275-c833f797780d
Local pid:
pubs:625356
Source identifiers:
625356
Deposit date:
2016-06-14

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