Publication | Open Access
Cross-regulation between Notch and p63 in keratinocyte commitment to differentiation
384
Citations
67
References
2006
Year
Cell SpecializationCellular PhysiologyTumor BiologyTranscriptional RegulationCell RegulationCell SignalingSkin DevelopmentP53 Family MemberCutaneous BiologyCell Cycle WithdrawalKeratinocyte CommitmentGene ExpressionCell BiologyLineage PlasticityDevelopmental BiologyTumor SuppressorMedicineCell DevelopmentHuman Keratinocytes
Notch signaling promotes commitment of keratinocytes to differentiation and suppresses tumorigenesis. p63, a p53 family member, has been implicated in establishment of the keratinocyte cell fate and/or maintenance of epithelial self-renewal. Here we show that p63 expression is suppressed by Notch1 activation in both mouse and human keratinocytes through a mechanism independent of cell cycle withdrawal and requiring down-modulation of selected interferon-responsive genes, including IRF7 and/or IRF3. In turn, elevated p63 expression counteracts the ability of Notch1 to restrict growth and promote differentiation. p63 functions as a selective modulator of Notch1-dependent transcription and function, with the Hes-1 gene as one of its direct negative targets. Thus, a complex cross-talk between Notch and p63 is involved in the balance between keratinocyte self-renewal and differentiation.
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