Résumé
The skin epidermis is an excellent example for exploring homeostasis and injury repair in a stratified epithelium. The epidermis maintains a single inner (basal) layer of proliferative cells that adhere to an underlying basement membrane rich in extracellular matrix (ECM) and growth factors (Fuchs 2007). Basal cells express a number of characteristic markers including keratins and transcription factors. Periodically, these cells withdraw from the cell cycle, commit to differentiate terminally, move outward and are eventually shed from the skin surface. This architecture allows the epidermis to generate a self-perpetuating barrier that keeps harmful microbes out and essential body fluids in.
Upon commitment to terminally differentiate, an epidermal keratinocyte progresses through three distinct differentiation stages: spinous, granular and stratum corneum. Major changes in transcription, morphology and function occur at the basal/spinous layer transition and again at the granular/stratum corneum transition, such that differentiated cells reaching the skin surface are enucleated, cellular skeletons that are packed with cables of keratin filaments encased by an indestructible envelope of proteins. An additional final step in the differentiation process is the extrusion of a lipid bilayer that seals and protects the body surface from dehydration and harmful microbes. The process is in a continual homeostasis, so that surface cells are continually sloughed and replaced by inner cells differentiating and moving outward. In human epidermis, the self-renewing capacity of epidermal stem cells is enormous, and within 4 weeks, a basal cell has terminally differentiated and exited at the skin surface. In mice, the epidermis becomes thinner and proliferation slows substantially as the hair coat develops.
