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JCS ePress online publication date 19 Aug 2008
doi: 10.1242/jcs.029256


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Research Article

HIF1 transcription factor regulates laminin-332 expression and keratinocyte migration


Giorgos Fitsialos, Isabelle Bourget, Séverine Augier, Amandine Ginouvès, Roger Rezzonico, Teresa Odorisio, Francesca Cianfarani, Thierry Virolle, Jacques Pouysségur, Guerrino Meneguzzi, Edurne Berra, Gilles Ponzio*, and Roser Buscà
* Author for correspondence (e-mail: ponzio{at}unice.fr)

Epidermal wound repair is a complex process involving the fine orchestrated regulation of crucial cell functions, such as proliferation, adhesion and migration. Using an in vitro model that recapitulates central aspects of epidermal wound healing, we demonstrate that the transcription factor HIF1 is strongly stimulated in keratinocyte cultures submitted to mechanical injury. Signals generated by scratch wounding stabilise the HIF1{alpha} protein, which requires activation of the PI3K pathway independently of oxygen availability. We further show that upregulation of HIF1{alpha} plays an essential role in keratinocyte migration during the in vitro healing process, because HIF1{alpha} inhibition dramatically delays the wound closure. In this context, we demonstrate that HIF1 controls the expression of laminin-332, one of the major epithelial cell adhesion ligands involved in cell migration and invasion. Indeed, silencing of HIF1{alpha} abrogates injury-induced laminin-332 expression, and we provide evidence that HIF1 directly regulates the promoter activity of the laminin {alpha}3 chain. Our results suggest that HIF1 contributes to keratinocyte migration and thus to the re-epithelialisation process by regulating laminin-332.


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