Fiche publication
Date publication
juin 2025
Journal
Aging cell
Auteurs
Membres identifiés du Cancéropôle Est :
Dr ROUGET Raphaël
Tous les auteurs :
Giroud J, Delvaux P, Carlier L, De Schutter C, Martin N, Rouget R, Bolouki A, De Glas V, Bouriez I, Bourdoux F, Burteau S, Théry J, Decanter G, Penel N, de Launoit Y, Ledoux B, Abbadie C, Poumay Y, Pluquet O, Debacq-Chainiaux F
Lien Pubmed
Résumé
Skin aging is influenced by both intrinsic and extrinsic factors, particularly UV radiation, and is characterized by an accumulation of senescent cells. Remarkably, exposure to UV can trigger senescence in different skin cell types, including dermal fibroblasts. However, the molecular mechanisms underlying UV-induced senescence and the impact of the related senescence-associated secretory phenotype (SASP) on the homeostasis of the overlying epidermis remain poorly understood. Here, we identified that both chronological aging and photoaging induce the unfolded protein response (UPR) in human dermal samples. We demonstrated that silencing ATF6α disrupts the establishment of the UVB-induced senescent phenotype by preventing the onset of several senescent biomarkers and alters the composition of the SASP, consequently affecting its impact on the increased proliferation of keratinocytes embedded in reconstructed human epidermis. Moreover, we found that ATF6α partially mediates IL8 expression involved in the hyperproliferation of cultured keratinocytes. Together, our findings highlight the importance of the ATF6α/IL8 axis in regulating the homeostasis of neighboring cells during skin photoaging, thus suggesting ATF6α as a potentially promising target for senotherapeutic interventions.
Mots clés
ATF6α, UPR, UVB‐induced senescence, normal human dermal fibroblasts, skin
Référence
Aging Cell. 2025 06;24(6):e70024
