期刊
IMMUNOLOGY LETTERS
卷 258, 期 -, 页码 8-19出版社
ELSEVIER
DOI: 10.1016/j.imlet.2023.04.009
关键词
NK cells; CD8+T cells; Hepatocellular carcinoma; NKp46; Tumor microenvironment
类别
This study showed that early removal of NK cells can significantly inhibit tumor growth in a CD8+T cell-dependent manner in a murine hepatocellular carcinoma model. The presence of abundant NKp46+ NK cells in the tumor microenvironment was positively correlated with tumor growth and these cells exhibited dysfunction. Blockade of NKp46 effectively attenuated HCC growth. This work revealed a regulatory role of tumor-associated NK cells in HCC and suggested NKp46 as a potential target for HCC treatment.
Natural killer(NK) cells comprise one subset of the innate lymphoid cells family. Despite reported anti-tumor activity of NK cells, their tangible contribution to tumor control remains controversial. This is due to the incomplete understanding of NK alterations within tumor microenvironment(TME). Here we showed, using murine hepatocellular carcinoma(HCC) model, that early NK cells deletion markedly attenuated tumor growth in a CD8+T cells dependent manner. This effect was accompanied by an enhanced CD8+T cells effector function in tumor rather than circulating blood. Then, we demonstrated that abundant NKp46+ NK subset, but not NKp46- NK, were recruited towards tumor microenvironment during tumor progression. Frequency of intratumor NKP46+ NK cells were inversely related to CD8+T cells activation, and positively correlated with tumor growth. Intratumor NKp46+ NK cells exhibited dysfunction and increased expression of inhibitory receptors, when compared with NKp46- NK cells. Blockade of NK cells-associated NKp46 effectively attenuated HCC growth. Infusion of tumor-derived NKp46+ NK cells markedly enhanced HCC growth in vivo, in contrast to tumor cells inoculation alone. The further mechanistic investigations unveiled that NK cells boosted tumor growth by NKp46-mediated impairment of CD8+T cells effector function. Overall, this work supported a previously unappreciated regulatory property of tumor-associated NK cells in HCC, and NKp46 as a potential target against HCC in clinical setting.
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