期刊
NATURE IMMUNOLOGY
卷 20, 期 8, 页码 1035-+出版社
NATURE PUBLISHING GROUP
DOI: 10.1038/s41590-019-0408-z
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资金
- American Heart Association [17POST33660907]
- National Institutes of Health [T32AI007509, AI132962, AI108765, AI104002, AI118916, AI083019, AI127463]
Type III interferon (IFN-lambda) is important for innate immune protection at mucosal surfaces and has therapeutic benefit against influenza A virus (IAV) infection. However, the mechanisms by which IFN-lambda programs adaptive immune protection against IAV are undefined. Here we found that IFN-lambda signaling in dendritic cell (DC) populations was critical for the development of protective IAV-specific CD8(+) T cell responses. Mice lacking the IFN-lambda receptor (Ifnlr1(-/-)) had blunted CD8(+) T cell responses relative to wild type and exhibited reduced survival after heterosubtypic IAV re-challenge. Analysis of DCs revealed IFN-lambda signaling directed the migration and function of CD103(+) DCs for development of optimal antiviral CD8(+) T cell responses, and bioinformatic analyses identified IFN-lambda regulation of a DC IL-10 immunoregulatory network. Thus, IFN-lambda serves a critical role in bridging innate and adaptive immunity from lung mucosa to lymph nodes to program DCs to direct effective T cell immunity against IAV.
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