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Decoding spatiotemporal transcriptional dynamics and epithelial fibroblast crosstalk during gastroesophageal junction development through single cell analysis

Author

Listed:
  • Naveen Kumar

    (Aarhus University
    University of Würzburg)

  • Pon Ganish Prakash

    (University of Würzburg)

  • Christian Wentland

    (University of Würzburg)

  • Shilpa Mary Kurian

    (University of Würzburg)

  • Gaurav Jethva

    (University of Würzburg)

  • Volker Brinkmann

    (Max Planck Institute for Infection Biology)

  • Hans-Joachim Mollenkopf

    (Max Planck Institute for Infection Biology)

  • Tobias Krammer

    (Helmholtz-Center for Infection Research (HZI))

  • Christophe Toussaint

    (Helmholtz-Center for Infection Research (HZI))

  • Antoine-Emmanuel Saliba

    (Helmholtz-Center for Infection Research (HZI)
    Institute of Molecular Infection Biology (IMIB))

  • Matthias Biebl

    (Charité University Medicine)

  • Christian Jürgensen

    (Charité University Medicine)

  • Bertram Wiedenmann

    (Charité University Medicine)

  • Thomas F. Meyer

    (Max Planck Institute for Infection Biology)

  • Rajendra Kumar Gurumurthy

    (University of Würzburg
    Max Planck Institute for Infection Biology)

  • Cindrilla Chumduri

    (Aarhus University
    University of Würzburg
    Max Planck Institute for Infection Biology
    Charité University Medicine)

Abstract

The gastroesophageal squamocolumnar junction (GE-SCJ) is a critical tissue interface between the esophagus and stomach, with significant relevance in the pathophysiology of gastrointestinal diseases. Despite this, the molecular mechanisms underlying GE-SCJ development remain unclear. Using single-cell transcriptomics, organoids, and spatial analysis, we examine the cellular heterogeneity and spatiotemporal dynamics of GE-SCJ development from embryonic to adult mice. We identify distinct transcriptional states and signaling pathways in the epithelial and mesenchymal compartments of the esophagus and stomach during development. Fibroblast-epithelial interactions are mediated by various signaling pathways, including WNT, BMP, TGF-β, FGF, EGF, and PDGF. Our results suggest that fibroblasts predominantly send FGF and TGF-β signals to the epithelia, while epithelial cells mainly send PDGF and EGF signals to fibroblasts. We observe differences in the ligands and receptors involved in cell-cell communication between the esophagus and stomach. Our findings provide insights into the molecular mechanisms underlying GE-SCJ development and fibroblast-epithelial crosstalk involved, paving the way to elucidate mechanisms during adaptive metaplasia development and carcinogenesis.

Suggested Citation

  • Naveen Kumar & Pon Ganish Prakash & Christian Wentland & Shilpa Mary Kurian & Gaurav Jethva & Volker Brinkmann & Hans-Joachim Mollenkopf & Tobias Krammer & Christophe Toussaint & Antoine-Emmanuel Sali, 2024. "Decoding spatiotemporal transcriptional dynamics and epithelial fibroblast crosstalk during gastroesophageal junction development through single cell analysis," Nature Communications, Nature, vol. 15(1), pages 1-20, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-47173-z
    DOI: 10.1038/s41467-024-47173-z
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