The lncRNA SNHG26 drives the inflammatory-to-proliferative state transition of keratinocyte progenitor cells during wound healing

The cell transitionfrom an inflammatory phase to a subsequent proliferative phase is crucial for wound healing, yet the driving mechanism remains unclear. By profiling lncRNA expression changesduring human skin wound healing and screening lncRNA functions, we identified SNHG26 as a pivotal regulator in keratinocyte progenitors underpinning this phase transition. Snhg26 -deficient mice exhibited impaired wound repair characterized by delayed re-epithelization accompanied by exacerbated inflammation. Single-cell transcriptome analysis combined with gain-of-function and loss-of-function of SNHG26 in vitro and ex vivo revealed its specific role in facilitating inflammatory-to-proliferative state transition of keratinocyte progenitors. A mechanistic study unraveled that SNHG26 interacted withand relocated the transcription factor ILF2 from inflammatory genomic loci, such as JUN, IL6, IL8, and CCL20 , to the genomic locus of LAMB3 . Collectively, our findings suggest that lncRNAs play cardinal roles in expediting tissue repair and regeneration and may constitute an invaluable reservoir of therapeutic targets in reparative medicine.