| Literature DB >> 30089718 |
Reiko Matsumoto1, Teruki Dainichi1, Soken Tsuchiya2, Takashi Nomura1, Akihiko Kitoh1, Matthew S Hayden3, Ken J Ishii4,5, Mayuri Tanaka4,5, Tetsuya Honda1, Gyohei Egawa1, Atsushi Otsuka1, Saeko Nakajima1, Kenji Sakurai1, Yuri Nakano1, Takashi Kobayashi6, Yukihiko Sugimoto2, Kenji Kabashima1,7.
Abstract
Epithelial cells are the first line of defense against external dangers, and contribute to induction of adaptive immunity including Th17 responses. However, it is unclear whether specific epithelial signaling pathways are essential for the development of robust IL-17-mediated immune responses. In mice, the development of psoriatic inflammation induced by imiquimod required keratinocyte TRAF6. Conditional deletion of TRAF6 in keratinocytes abrogated dendritic cell activation, IL-23 production, and IL-17 production by γδ T cells at the imiquimod-treated sites. In contrast, hapten-induced contact hypersensitivity and papain-induced IgE production were not affected by loss of TRAF6. Loss of psoriatic inflammation was not solely due to defective imiquimod sensing, as subcutaneous administration of IL-23 restored IL-17 production but did not reconstitute psoriatic pathology in the mutant animals. Thus, TRAF6 was required for the full development of IL-17-mediated inflammation. Therefore, epithelial TRAF6 signaling plays an essential role in both triggering and propagating IL-17-mediated psoriatic inflammation.Entities:
Keywords: Cellular immune response; Dermatology; Immunology; Skin
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Year: 2018 PMID: 30089718 PMCID: PMC6129131 DOI: 10.1172/jci.insight.121175
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708