A circulating subset of iNKT cells mediates antitumor and antiviral immunity

免疫学 生物 自然杀伤性T细胞 免疫系统 先天免疫系统 细胞生物学 CD8型
作者
Guangwei Cui,Akihiro Shimba,Jianshi Jin,Taisaku Ogawa,Yukiko Muramoto,Hitoshi Miyachi,Shinya Abe,T. Asahi,Shizue Tani‐ichi,Johannes M. Dijkstra,Yayoi Iwamoto,Kirill Kryukov,Yuanbo Zhu,Daichi Takami,Takahiro Hara,Satsuki Kitano,Yan Xu,Hajime Morita,Moyu Zhang,Lynn Zreka,Keishi Miyata,Takashi Kanaya,Shinya Okumura,Takashi Ito,Etsuro Hatano,Yoshimasa Takahashi,Hiroshi Watarai,Yuichi Oike,Tadashi Imanishi,Hiroshi Ohno,Toshiaki Ohteki,Nagahiro Minato,Masato Kubo,Georg A. Holländer,Hideki Ueno,Takeshi Noda,Katsuyuki Shiroguchi,Koichi Ikuta
出处
期刊:Science immunology [American Association for the Advancement of Science]
卷期号:7 (76) 被引量:31
标识
DOI:10.1126/sciimmunol.abj8760
摘要

Invariant natural killer T (iNKT) cells are a group of innate-like T lymphocytes that recognize lipid antigens. They are supposed to be tissue resident and important for systemic and local immune regulation. To investigate the heterogeneity of iNKT cells, we recharacterized iNKT cells in the thymus and peripheral tissues. iNKT cells in the thymus were divided into three subpopulations by the expression of the natural killer cell receptor CD244 and the chemokine receptor CXCR6 and designated as C0 (CD244-CXCR6-), C1 (CD244-CXCR6+), or C2 (CD244+CXCR6+) iNKT cells. The development and maturation of C2 iNKT cells from C0 iNKT cells strictly depended on IL-15 produced by thymic epithelial cells. C2 iNKT cells expressed high levels of IFN-γ and granzymes and exhibited more NK cell-like features, whereas C1 iNKT cells showed more T cell-like characteristics. C2 iNKT cells were influenced by the microbiome and aging and suppressed the expression of the autoimmune regulator AIRE in the thymus. In peripheral tissues, C2 iNKT cells were circulating that were distinct from conventional tissue-resident C1 iNKT cells. Functionally, C2 iNKT cells protected mice from the tumor metastasis of melanoma cells by enhancing antitumor immunity and promoted antiviral immune responses against influenza virus infection. Furthermore, we identified human CD244+CXCR6+ iNKT cells with high cytotoxic properties as a counterpart of mouse C2 iNKT cells. Thus, this study reveals a circulating subset of iNKT cells with NK cell-like properties distinct from conventional tissue-resident iNKT cells.
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