Abstract
Local hypoxia is general consequence of an acute skin wound due to vascular disruption and high oxygen consumption by cells at the edge of the wound. The resident γδ T cells in the skin, Dendritic Epidermal T Cells (DETC), are known to support local tissue homeostasis and wound repair by local production of growth factors, such as keratinocyte growth factors (KGFs) and insulin‐like growth factor (IGF)‐1. We have analyzed the functional role of DETC in response to local tissue hypoxia generated by an acute skin wound. The hypoxic status of the skin wound induced HIF‐1α expression in DETC. HIF‐1α signalling during hypoxia induced expression of vascular endothelial growth factor (VEGF) by DETC. Wound healing was impaired after HIF‐1α gene‐silencing in DETC and this impairment was rescued by VEGF administration. Together this data demonstrates that acute skin wound induces HIF‐1α signaling in DETC, which promote VEGF production with the result of enhancing skin wound healing.Grant: NIH‐AI‐36964
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