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Dedifferentiation maintains melanocyte stem cells in a dynamic niche

Author

Listed:
  • Qi Sun

    (New York University Grossman School of Medicine)

  • Wendy Lee

    (New York University Grossman School of Medicine)

  • Hai Hu

    (New York University Grossman School of Medicine)

  • Tatsuya Ogawa

    (New York University Grossman School of Medicine)

  • Sophie Leon

    (New York University Grossman School of Medicine)

  • Ioanna Katehis

    (New York University Grossman School of Medicine)

  • Chae Ho Lim

    (New York University Grossman School of Medicine)

  • Makoto Takeo

    (New York University Grossman School of Medicine)

  • Michael Cammer

    (New York University Grossman School of Medicine)

  • M. Mark Taketo

    (Kyoto University Hospital–iACT, Kyoto University)

  • Denise L. Gay

    (New York University Grossman School of Medicine
    DLGBioLogics)

  • Sarah E. Millar

    (Icahn School of Medicine at Mount Sinai)

  • Mayumi Ito

    (New York University Grossman School of Medicine)

Abstract

For unknow reasons, the melanocyte stem cell (McSC) system fails earlier than other adult stem cell populations1, which leads to hair greying in most humans and mice2,3. Current dogma states that McSCs are reserved in an undifferentiated state in the hair follicle niche, physically segregated from differentiated progeny that migrate away following cues of regenerative stimuli4–8. Here we show that most McSCs toggle between transit-amplifying and stem cell states for both self-renewal and generation of mature progeny, a mechanism fundamentally distinct from those of other self-renewing systems. Live imaging and single-cell RNA sequencing revealed that McSCs are mobile, translocating between hair follicle stem cell and transit-amplifying compartments where they reversibly enter distinct differentiation states governed by local microenvironmental cues (for example, WNT). Long-term lineage tracing demonstrated that the McSC system is maintained by reverted McSCs rather than by reserved stem cells inherently exempt from reversible changes. During ageing, there is accumulation of stranded McSCs that do not contribute to the regeneration of melanocyte progeny. These results identify a new model whereby dedifferentiation is integral to homeostatic stem cell maintenance and suggest that modulating McSC mobility may represent a new approach for the prevention of hair greying.

Suggested Citation

  • Qi Sun & Wendy Lee & Hai Hu & Tatsuya Ogawa & Sophie Leon & Ioanna Katehis & Chae Ho Lim & Makoto Takeo & Michael Cammer & M. Mark Taketo & Denise L. Gay & Sarah E. Millar & Mayumi Ito, 2023. "Dedifferentiation maintains melanocyte stem cells in a dynamic niche," Nature, Nature, vol. 616(7958), pages 774-782, April.
  • Handle: RePEc:nat:nature:v:616:y:2023:i:7958:d:10.1038_s41586-023-05960-6
    DOI: 10.1038/s41586-023-05960-6
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