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A transcriptional network governing ceramide homeostasis establishes a cytokine-dependent developmental process

Author

Listed:
  • Ruiqi Liao

    (University of Wisconsin School of Medicine and Public Health)

  • Abiola Babatunde

    (University of Wisconsin School of Medicine and Public Health)

  • Stephanie Qiu

    (University of Wisconsin School of Medicine and Public Health)

  • Hamsini Harikumar

    (University of Wisconsin School of Medicine and Public Health)

  • Joshua J. Coon

    (University of Wisconsin School of Medicine and Public Health
    Morgridge Institute for Research
    University of Wisconsin-Madison)

  • Katherine A. Overmyer

    (University of Wisconsin School of Medicine and Public Health
    Morgridge Institute for Research)

  • Yusuf A. Hannun

    (Stony Book University
    Northport Veterans Affairs Medical Center)

  • Chiara Luberto

    (Stony Brook University)

  • Emery H. Bresnick

    (University of Wisconsin School of Medicine and Public Health)

Abstract

Transcriptional mechanisms controlling developmental processes establish and maintain proteomic networks, which can govern the levels of intracellular small molecules. Although dynamic changes in bioactive small molecules can link transcription factor and genome activity with cell state transitions, many mechanistic questions are unresolved. Using quantitative lipidomics and multiomics, we discover that the hematopoietic transcription factor GATA1 establishes ceramide homeostasis during erythroid differentiation by regulating genes encoding sphingolipid metabolic enzymes. Inhibiting a GATA1-induced sphingolipid biosynthetic enzyme, delta(4)-desaturase, or disrupting ceramide homeostasis with cell-permeable dihydroceramide or ceramide is detrimental to erythroid, but not myeloid, progenitor activity. Coupled with genetic editing-based rewiring of the regulatory circuitry, we demonstrate that ceramide homeostasis commissions vital stem cell factor and erythropoietin signaling by opposing an inhibitory protein phosphatase 2A-dependent, dual-component mechanism. Integrating bioactive lipids as essential components of GATA factor mechanisms to control cell state transitions has implications for diverse cell and tissue types.

Suggested Citation

  • Ruiqi Liao & Abiola Babatunde & Stephanie Qiu & Hamsini Harikumar & Joshua J. Coon & Katherine A. Overmyer & Yusuf A. Hannun & Chiara Luberto & Emery H. Bresnick, 2023. "A transcriptional network governing ceramide homeostasis establishes a cytokine-dependent developmental process," Nature Communications, Nature, vol. 14(1), pages 1-16, December.
  • Handle: RePEc:nat:natcom:v:14:y:2023:i:1:d:10.1038_s41467-023-42978-w
    DOI: 10.1038/s41467-023-42978-w
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