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Chondrocytes in the resting zone of the growth plate are maintained in a Wnt-inhibitory environment.

Shawn A HallettYuki MatsushitaWanida OnoNaoko SakagamiKoji MizuhashiNicha TokavanichMizuki NagataAnnabelle ZhouTakao HiraiHenry M KronenbergNoriaki Ono
Published in: eLife (2021)
Chondrocytes in the resting zone of the postnatal growth plate are characterized by slow cell cycle progression, and encompass a population of parathyroid hormone-related protein (PTHrP)-expressing skeletal stem cells that contribute to the formation of columnar chondrocytes. However, how these chondrocytes are maintained in the resting zone remains undefined. We undertook a genetic pulse-chase approach to isolate slow cycling, label-retaining chondrocytes (LRCs) using a chondrocyte-specific doxycycline-controllable Tet-Off system regulating expression of histone 2B-linked GFP. Comparative RNA-seq analysis identified significant enrichment of inhibitors and activators for Wnt signaling in LRCs and non-LRCs, respectively. Activation of Wnt/β-catenin signaling in PTHrP+ resting chondrocytes using Pthlh-creER and Apc-floxed allele impaired their ability to form columnar chondrocytes. Therefore, slow-cycling chondrocytes are maintained in a Wnt-inhibitory environment within the resting zone, unraveling a novel mechanism regulating maintenance and differentiation of PTHrP+ skeletal stem cells of the postnatal growth plate.
Keyphrases
  • stem cells
  • heart rate
  • cell cycle
  • extracellular matrix
  • heart rate variability
  • cell proliferation
  • rna seq
  • single cell
  • blood pressure
  • dna methylation
  • genome wide
  • high intensity
  • gene expression
  • binding protein