Homeostatic IL-13 in healthy skin directs dendritic cell differentiation to promote TH2 and inhibit TH17 cell polarization

Innate lymphoid cells;先天淋巴细胞;Cellular immunity;细胞免疫;Conventional dendritic cells;常规树突状细胞;树突状细胞;IL-13;dendritic cell differentiation;树突状细胞分化;TH2;TH17 cell polarization;细胞极化
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Johannes U Mayer, Kerry L Hilligan, Jodie S Chandler, David A Eccles, Samuel I Old, Rita G Domingues, Jianping Yang, Greta R Webb, Luis Munoz-Erazo, Evelyn J Hyde, Kirsty A Wakelin, Shiau-Choot Tang, Sally C Chappell, Sventja von Daake, Frank Brombacher, Charles R Mackay, Alan Sher, Roxane Tussiwand, Lisa M Connor, David Gallego-Ortega, Dragana Jankovic, Graham Le Gros, Matthew R Hepworth, Olivier Lamiable #, Franca Ronchese #

  • Nat Immunol
  • 2021
  • 31.25
  • 22(12):1538-1550
  • Mouse
  • 单细胞测序
  • frozen cell pellets
  • 免疫/内分泌
  • 树突状细胞,T细胞

Abstract

Abstract

The signals driving the adaptation of type 2 dendritic cells (DC2s) to diverse peripheral environments remain mostly undefined. We show that differentiation of CD11blo migratory DC2s-a DC2 population unique to the dermis-required IL-13 signaling dependent on the transcription factors STAT6 and KLF4, whereas DC2s in lung and small intestine were STAT6-independent. Similarly, human DC2s in skin expressed an IL-4 and IL-13 gene signature that was not found in blood, spleen and lung DCs. In mice, IL-13 was secreted homeostatically by dermal innate lymphoid cells and was independent of microbiota, TSLP or IL-33. In the absence of IL-13 signaling, dermal DC2s were stable in number but remained CD11bhi and showed defective activation in response to allergens, with diminished ability to support the development of IL-4+GATA3+ helper T cells (TH), whereas antifungal IL-17+RORγt+ TH cells were increased. Therefore, homeostatic IL-13 fosters a noninflammatory skin environment that supports allergic sensitization.
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