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Cellular transitions during cranial suture establishment in zebrafish

Author

Listed:
  • D’Juan T. Farmer

    (University of California)

  • Jennifer E. Dukov

    (University of California)

  • Hung-Jhen Chen

    (University of California)

  • Claire Arata

    (University of Southern California)

  • Jose Hernandez-Trejo

    (University of Southern California)

  • Pengfei Xu

    (University of California, San Francisco)

  • Camilla S. Teng

    (University of California San Francisco)

  • Robert E. Maxson

    (University of Southern California)

  • J. Gage Crump

    (University of Southern California)

Abstract

Cranial sutures separate neighboring skull bones and are sites of bone growth. A key question is how osteogenic activity is controlled to promote bone growth while preventing aberrant bone fusions during skull expansion. Using single-cell transcriptomics, lineage tracing, and mutant analysis in zebrafish, we uncover key developmental transitions regulating bone formation at sutures during skull expansion. In particular, we identify a subpopulation of mesenchyme cells in the mid-suture region that upregulate a suite of genes including BMP antagonists (e.g. grem1a) and pro-angiogenic factors. Lineage tracing with grem1a:nlsEOS reveals that this mid-suture subpopulation is largely non-osteogenic. Moreover, combinatorial mutation of BMP antagonists enriched in this mid-suture subpopulation results in increased BMP signaling in the suture, misregulated bone formation, and abnormal suture morphology. These data reveal establishment of a non-osteogenic mesenchyme population in the mid-suture region that restricts bone formation through local BMP antagonism, thus ensuring proper suture morphology.

Suggested Citation

  • D’Juan T. Farmer & Jennifer E. Dukov & Hung-Jhen Chen & Claire Arata & Jose Hernandez-Trejo & Pengfei Xu & Camilla S. Teng & Robert E. Maxson & J. Gage Crump, 2024. "Cellular transitions during cranial suture establishment in zebrafish," Nature Communications, Nature, vol. 15(1), pages 1-16, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-50780-5
    DOI: 10.1038/s41467-024-50780-5
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