Abstract EN:

The autophagy constitutes a mechanism with apoptosis implied in the control of cell homeostasis, owing to its involvement in the degradation and the renewal of macromolecules and organelles. This process would intervene during differentiation. Firstly, we studied if the induction of differentiation was linked to an activation of autophagy in keratinocytes. From the first hours of the differentiation, there is an initiation of autophagy. The progress of the events, in time, is characterized by modifications of markers of expression (Sirt1, mTOR, Beclin-1, LC3-II, etc. ). Secondly, we characterized oxidative moderate stress induced autophagy in HaCaT keratinocytes. For moderated stress, autophagy (via p62, Beclin-1, LC3-II…) eliminates the damaged constituents. The inhibition of autophagy, by pharmacological drug (3MA) or extinction of p62 protein, confirms the obtained results. On the other hand, a lesser activation of autophagy of keratinocytes isolated old subjects in comparison with cells from young subjets, supported that with age the efficiency to remove damage was altered. The preservation of these capacities constitutes an evident stake, in particular, for the cosmeto-dermatology.