| Literature DB >> 29174333 |
Levi Gadye1, Diya Das2, Michael A Sanchez3, Kelly Street4, Ariane Baudhuin3, Allon Wagner5, Michael B Cole6, Yoon Gi Choi7, Nir Yosef5, Elizabeth Purdom8, Sandrine Dudoit9, Davide Risso10, John Ngai11, Russell B Fletcher3.
Abstract
Tissue homeostasis and regeneration are mediated by programs of adult stem cell renewal and differentiation. However, the mechanisms that regulate stem cell fates under such widely varying conditions are not fully understood. Using single-cell techniques, we assessed the transcriptional changes associated with stem cell self-renewal and differentiation and followed the maturation of stem cell-derived clones using sparse lineage tracing in the regenerating mouse olfactory epithelium. Following injury, quiescent olfactory stem cells rapidly shift to activated, transient states unique to regeneration and tailored to meet the demands of injury-induced repair, including barrier formation and proliferation. Multiple cell fates, including renewed stem cells and committed differentiating progenitors, are specified during this early window of activation. We further show that Sox2 is essential for cells to transition from the activated to neuronal progenitor states. Our study highlights strategies for stem cell-mediated regeneration that may be conserved in other adult stem cell niches.Entities:
Keywords: cell fate; cell state; lineage; lineage tracing; olfactory; regeneration; scRNA-seq; stem cells
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Year: 2017 PMID: 29174333 PMCID: PMC5728414 DOI: 10.1016/j.stem.2017.10.014
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633