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Transcriptional dynamics of the oligodendrocyte lineage and its regulation by the brain erythropoietin system

Author

Listed:
  • Liu Ye

    (City Campus
    Guangxi Medical University Cancer Hospital)

  • Vinicius Daguano Gastaldi

    (City Campus
    Georg-August-University)

  • Yasmina Curto

    (City Campus)

  • Anne-Fleur Wildenburg

    (City Campus
    Georg-August-University
    City Campus)

  • Xuan Yu

    (City Campus
    Georg-August-University
    City Campus)

  • Martin Hindermann

    (City Campus
    Georg-August-University)

  • Simone Eggert

    (City Campus)

  • Anja Ronnenberg

    (City Campus)

  • Qing Wang

    (University of California Los Angeles)

  • Umer Javed Butt

    (City Campus)

  • Riki Kawaguchi

    (University of California Los Angeles)

  • Daniel Geschwind

    (University of California Los Angeles)

  • Wiebke Möbius

    (City Campus)

  • Susann Boretius

    (Leibniz Institute for Primate Research)

  • Manvendra Singh

    (City Campus
    Heidelberg University)

  • Klaus-Armin Nave

    (City Campus)

  • Hannelore Ehrenreich

    (City Campus
    Georg-August-University
    Heidelberg University)

Abstract

Oligodendrocytes differentiate from oligodendrocyte progenitor cells (OPC) in early postnatal development, but some oligodendrogenesis is maintained throughout adulthood, where oligodendrocyte lineage dynamics may contribute to neuroplasticity, adaptive myelination, and myelin repair. Here, we studied the effect of erythropoietin (EPO) and its receptor (EPOR) on oligodendrocyte lineage dynamics employing murine hippocampus and its myelinated fibers as model region. Using multiple stage-specific markers and single-nuclei-RNA-seq data, we find that EPO stimulates all oligodendroglial lineage cells directly, driving differentiation/maturation. Differential gene expression analysis reveals multiple EPO-regulated mRNAs, including downregulated transcripts for GABA-A receptors, fitting the known inhibition of oligodendrocyte maturation by GABA. Importantly, analogous oligodendrocyte responses are seen when endogenous EPO expression in brain is stimulated by hypoxia. Mice lacking EPOR from mature oligodendrocytes show subtle deficiencies of adult myelination in hippocampal fimbria and mild working memory deficits. These gain- and loss-of-function experiments may further suggest EPO as clinically safe treatment for remyelination therapies.

Suggested Citation

  • Liu Ye & Vinicius Daguano Gastaldi & Yasmina Curto & Anne-Fleur Wildenburg & Xuan Yu & Martin Hindermann & Simone Eggert & Anja Ronnenberg & Qing Wang & Umer Javed Butt & Riki Kawaguchi & Daniel Gesch, 2025. "Transcriptional dynamics of the oligodendrocyte lineage and its regulation by the brain erythropoietin system," Nature Communications, Nature, vol. 16(1), pages 1-20, December.
  • Handle: RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-62791-x
    DOI: 10.1038/s41467-025-62791-x
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