4.8 Article

The circadian molecular clock creates epidermal stem cell heterogeneity

Journal

NATURE
Volume 480, Issue 7376, Pages 209-U89

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/nature10649

Keywords

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Funding

  1. AICR (Association for International Cancer Research)
  2. Spanish Ministry of Health (FIS)
  3. AGAUR (Agencia de Gestio d'Ajuts Universitaris i de Recerca
  4. Government of Cataluna)
  5. AGAUR
  6. FIS
  7. ICREA Funding Source: Custom
  8. Worldwide Cancer Research [10-0177] Funding Source: researchfish

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Murine epidermal stem cells undergo alternate cycles of dormancy and activation, fuelling tissue renewal. However, only a subset of stem cells becomes active during each round of morphogenesis, indicating that stem cells coexist in heterogeneous responsive states. Using a circadian-clock reporter-mouse model, here we show that the dormant hair-follicle stem cell niche contains coexisting populations of cells at opposite phases of the clock, which are differentially predisposed to respond to homeostatic cues. The core clock protein Bmal1 modulates the expression of stem cell regulatory genes in an oscillatory manner, to create populations that are either predisposed, or less prone, to activation. Disrupting this clock equilibrium, through deletion of Bmal1 (also known as Arntl) or Per1/2, resulted in a progressive accumulation or depletion of dormant stem cells, respectively. Stem cell arrhythmia also led to premature epidermal ageing, and a reduction in the development of squamous tumours. Our results indicate that the circadian clock fine-tunes the temporal behaviour of epidermal stem cells, and that its perturbation affects homeostasis and the predisposition to tumorigenesis.

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