4.7 Article

Coordinated changes in cellular behavior ensure the lifelong maintenance of the hippocampal stem cell population

期刊

CELL STEM CELL
卷 28, 期 5, 页码 863-+

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CELL PRESS
DOI: 10.1016/j.stem.2021.01.003

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资金

  1. Francis Crick Institute from Cancer Research UK [FC0010089]
  2. UK Medical Research Council [FC0010089, U117570528]
  3. Wellcome Trust [FC0010089, 106187/Z/14/Z]
  4. German Research Foundation (DFG) [SFB 873]
  5. Wellcome Trust [106187/Z/14/Z] Funding Source: Wellcome Trust
  6. MRC [MR/M023907/1, MC_U117570528] Funding Source: UKRI

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The stabilization of neural stem cell numbers in young adults is a result of coordinated changes in stem cell behavior, with resting cells having a higher activation rate and greater contribution to neurogenesis. This change is associated with a progressive reduction in expression of the pro-activation protein ASCL1 due to increased post-translational degradation, providing insights into hippocampal NSC dynamics and neurogenesis rates in different mammalian species, including humans.
Neural stem cell numbers fall rapidly in the hippocampus of juvenile mice but stabilize during adulthood, ensuring lifelong hippocampal neurogenesis. We show that this stabilization of stem cell numbers in young adults is the result of coordinated changes in stem cell behavior Although proliferating neural stem cells in juveniles differentiate rapidly, they increasingly return to a resting state of shallow quiescence and progress through additional self-renewing divisions in adulthood. Single-cell transcriptomics, modeling, and label retention analyses indicate that resting cells have a higher activation rate and greater contribution to neurogenesis than dormant cells, which have not left quiescence. These changes in stem cell behavior result from a progressive reduction in expression of the pro-activation protein ASCL1 because of increased post-translational degradation. These cellular mechanisms help reconcile current contradictory models of hippocampal neural stem cell (NSC) dynamics and may contribute to the different rates of decline of hippocampal neurogenesis in mammalian species, including humans.

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