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CD160 is essential for NK-mediated IFN-gamma production

Authors
Tu, Tony C.Brown, Nicholas K.Kim, Tae-JinWroblewska, JoannaYang, XuanmingGuo, XiaohuanLee, Seoyun HyunjiKumar, VinayLee, Kyung-MiFu, Yang-Xin
Issue Date
Mar-2015
Publisher
ROCKEFELLER UNIV PRESS
Citation
JOURNAL OF EXPERIMENTAL MEDICINE, v.212, no.3, pp.415 - 429
Indexed
SCIE
SCOPUS
Journal Title
JOURNAL OF EXPERIMENTAL MEDICINE
Volume
212
Number
3
Start Page
415
End Page
429
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/94207
DOI
10.1084/jem.20131601
ISSN
0022-1007
Abstract
NK-derived cytokines play important roles for natural killer (NK) function, but how the cytokines are regulated is poorly understood. CD160 is expressed on activated NK or T cells in humans but its function is unknown. We generated CD160-deficient mice to probe its function. Although CD160(-/-) mice showed no abnormalities in lymphocyte development, the control of NK-sensitive tumors was severely compromised in CD160(-/-) mice. Surprisingly, the cytotoxicity of NK cells was not impaired, but interferon-gamma (IFN-gamma) secretion by NK cells was markedly reduced in CD160(-/-) mice. Functionally targeting CD160 signaling with a soluble CD160-Ig also impaired tumor control and IFN-gamma production, suggesting an active role of CD160 signaling. Using reciprocal bone marrow transfer and cell culture, we have identified the intrinsic role of CD160 on NK cells, as well as its receptor on non-NK cells, for regulating cytokine production. To demonstrate sufficiency of the CD160(+) NK cell subset in controlling NK-dependent tumor growth, intratumoral transfer of the CD160(+) NK fraction led to tumor regression in CD160(-/-) tumor-bearing mice, indicating demonstrable therapeutic potential for controlling early tumors. Therefore, CD160 is not only an important biomarker but also functionally controls cytokine production by NK cells.
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