4.7 Article

Bone morphology is regulated modularly by global and regional genetic programs

Journal

DEVELOPMENT
Volume 146, Issue 14, Pages -

Publisher

COMPANY BIOLOGISTS LTD
DOI: 10.1242/dev.167882

Keywords

Cartilage; Patterning; Morphology; Superstructure; Sox9; Scleraxis; Modularity; Gli3; Pbx; Hox; Mouse

Funding

  1. National Institutes of Health [R01 AR055580]
  2. European Research Council [310098]
  3. Jeanne and Joseph Nissim Foundation for Life Sciences Research
  4. Y. Leon Benoziyo Institute for Molecular Medicine, Beth Rom-Rymer
  5. Estate of David Levinson
  6. Jaffe Bernard and Audrey Foundation
  7. Georges Lustgarten Cancer Research Fund
  8. David and Fela Shapell Family Center for Genetic Disorders
  9. David and Fela Shapell Family Foundation INCPM Fund for Preclinical Studies
  10. Estate of Bernard Bishin for the WIS-Clalit Program
  11. European Research Council (ERC) [310098] Funding Source: European Research Council (ERC)

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Bone protrusions provide stable anchoring sites for ligaments and tendons and define the unique morphology of each long bone. Despite their importance, the mechanism by which superstructures are patterned is unknown. Here, we identify components of the genetic program that control the patterning of Sox9(+)/Scx(+ )superstructure progenitors in mouse and show that this program includes both global and regional regulatory modules. Using light-sheet fluorescence microscopy combined with genetic lineage labeling, we mapped the broad contribution of the Sox9(+)/Scx(+) progenitors to the formation of bone superstructures. Then, by combining literature-based evidence, comparative transcriptomic analysis and genetic mouse models, we identified Gli3 as a global regulator of superstructure patterning, whereas Pbx1, Pbx2, Hoxa11 and Hoxd11 act as proximal and distal regulators, respectively. Moreover, by demonstrating a dose-dependent pattern regulation in Gli3 and Pbx1 compound mutations, we show that the global and regional regulatory modules work in a coordinated manner. Collectively, our results provide strong evidence for genetic regulation of superstructure patterning, which further supports the notion that long bone development is a modular process.

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