Cell Reports
Volume 21, Issue 8, 21 November 2017, Pages 2236-2250
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Article
Niche Cadherins Control the Quiescence-to-Activation Transition in Muscle Stem Cells

https://doi.org/10.1016/j.celrep.2017.10.102Get rights and content
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Highlights

  • Niche cadherins regulate muscle stem cell (SC) quiescence

  • Expansion of a regeneration-proficient SC pool associated with loss of cadherins

  • Cadherin-deficient SCs enter a state of partial activation

  • Nuclear β-catenin signaling is a necessary downstream driver of these phenotypes

Summary

Many adult stem cells display prolonged quiescence, promoted by cues from their niche. Upon tissue damage, a coordinated transition to the activated state is required because non-physiological breaks in quiescence often lead to stem cell depletion and impaired regeneration. Here, we identify cadherin-mediated adhesion and signaling between muscle stem cells (satellite cells [SCs]) and their myofiber niche as a mechanism that orchestrates the quiescence-to-activation transition. Conditional removal of N-cadherin and M-cadherin in mice leads to a break in SC quiescence, with long-term expansion of a regeneration-proficient SC pool. These SCs have an incomplete disruption of the myofiber-SC adhesive junction and maintain niche residence and cell polarity, yet show properties of SCs in a state of transition from quiescence toward full activation. Among these is nuclear localization of β-catenin, which is necessary for this phenotype. Injury-induced perturbation of niche adhesive junctions is therefore a likely first step in the quiescence-to-activation transition.

Keywords

stem cell
niche
muscle
satellite cell
cell adhesion
quiescence
regeneration
cadherin
β-catenin

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