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Diminished γδ T Cells during Murine Allergic Skin Inflammation Is Mediated by IL-4 Signaling in Keratinocytes. | LitMetric

AI Article Synopsis

  • Atopic dermatitis leads to weakened skin barrier and changes in antimicrobial peptide production, with dendritic epidermal T cells (DETCs) crucial for healing and inflammation.
  • Researchers found that mice lacking the IL-4 receptor (Il4ra-/-) showed higher DETC levels, quicker wound healing, and better skin repair gene expression compared to normal mice.
  • The study highlights that IL-4's negative impact on DETCs in allergic skin inflammation is primarily due to its effects on keratinocytes, where a lack of IL-4Rα boosts DETC numbers and reduces inflammation.

Article Abstract

Atopic dermatitis results in diminished barrier function and altered production of antimicrobial peptides. Dendritic epidermal T cells (DETCs) play an important role in the wound repair and inflammation process. Our previous work identified an IL-4-dependent loss of DETCs in Stat6VT mice and in the MC903-induced skin inflammation mouse model. However, the mechanisms through which IL-4 mediates the loss of DETCs are unclear. In this study, we show that IL-4Rα germline knockout mice (Il4ra-/-) have increased DETCs, faster wound healing, and increased epidermal differentiation complex gene and fibronectin expression. The absence of IL-4Rα minimized the MC903-induced loss of DETCs, and reciprocal bone marrow chimera experiments in Il4ra-/- and wild-type mice demonstrated structural nonhematopoietic IL-4-responsive cell-mediated DETC homeostasis. Skin keratinocyte-derived IL-15 decreased dramatically in the MC903 model, while injection of IL-15 rescued DETC loss by promoting DETC proliferation and limiting apoptosis. Conditional deletion of IL-4Rα from keratinocytes using Il4rafl/fl K14-Cre mice showed an increase of DETCs, increased IL-15 production, and diminished skin inflammation following wounding. These results suggest that IL-4-dependent effects on DETCs in allergic skin inflammation are mediated by the IL-4Rα receptor of keratinocytes.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11343438PMC
http://dx.doi.org/10.4049/jimmunol.2300629DOI Listing

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