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Letter
Nature 452, 225-229 (13 March 2008) | doi:10.1038/nature06642; Received 9 August 2007; Accepted 8 January 2008; Published online 2 March 2008
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A skin microRNA promotes differentiation by repressing 'stemness'
Rui Yi1,2, Matthew N. Poy3, Markus Stoffel3 & Elaine Fuchs1,2
- Howard Hughes Medical Institute, and,
- Laboratory of Mammalian Cell Biology and Development, The Rockefeller University, New York City, New York 10065, USA
- Swiss Federal Institute of Technology ETH Zurich, Institute of Molecular Systems Biology, CH-8093 Zürich, Switzerland
Correspondence to: Elaine Fuchs1,2 Correspondence and requests for materials should be addressed to E.F. (Email: fuchslb@rockefeller.edu).
Abstract
In stratified epithelial tissues, homeostasis relies on the self-renewing capacity of stem cells located within the innermost basal layer1. As basal cells become suprabasal, they lose proliferative potential and embark on a terminal differentiation programme2, 3. Here, we show that microRNA-203 is induced in the skin concomitantly with stratification and differentiation. By altering miR-203's spatiotemporal expression in vivo, we show that miR-203 promotes epidermal differentiation by restricting proliferative potential and inducing cell-cycle exit. We identify p63 as one of the conserved targets of miR-203 across vertebrates. Notably, p63 is an essential regulator of stem-cell maintenance in stratified epithelial tissues4, 5, 6, 7, 8, 9. We show that miR-203 directly represses the expression of p63: it fails to switch off suprabasally when either Dicer1 or miR-203 is absent and it becomes repressed basally when miR-203 is prematurely expressed. Our findings suggest that miR-203 defines a molecular boundary between proliferative basal progenitors and terminally differentiating suprabasal cells, ensuring proper identity of neighbouring layers.
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