High-dose NB-UVB exacerbates vitiligo progression by inducing dermal fibroblast senescence via the p38 MAPK signaling pathway - PubMed

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High-dose NB-UVB exacerbates vitiligo progression by inducing dermal fibroblast senescence via the p38 MAPK signaling pathway.
Dermal fibroblasts play a key role in vitiligo by responding to IFN-γ and secreting chemokines to recruit and activate CD8+ T cells.
NB-UVB irradiation induces dermal fibroblast senescence and activates both the MAPK and p53 pathways.
In vitro, high-dose NB-UVB exposure leads to increased senescence and inflammation in vitiligo fibroblasts.
Low-dose NB-UVB treatment in vitiligo mice reduces CD8+ T cells and increases skin pigmentation.
High-dose NB-UVB induces a senescent, proinflammatory microenvironment, disrupting skin homeostasis and exacerbating vitiligo progression.

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