Published July 25, 2019
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Data from: Wnt/PCP controls spreading of Wnt/β-catenin signals by cytonemes in vertebrates
Authors/Creators
- 1. University of Exeter
- 2. Karlsruhe Institute of Technology
- 3. University Hospital Heidelberg
- 4. John von Neumann Institute for Computing
- 5. Heidelberg University
- 6. University of Illinois at Urbana Champaign
Description
Signaling filopodia, termed cytonemes, are dynamic actin-based membrane structures that regulate the exchange of signaling molecules and their receptors within tissues. However, how cytoneme formation is regulated remains unclear. Here, we show that Wnt/PCP autocrine signaling controls the emergence of cytonemes, and that cytonemes subsequently control paracrine Wnt/β-catenin signal activation. Upon binding of the Wnt family member Wnt8a, the receptor tyrosine kinase Ror2 gets activated. Ror2/PCP signaling leads to induction of cytonemes, which mediate transport of Wnt8a to neighboring cells. In the Wnt receiving cells, Wnt8a on cytonemes triggers Wnt/β-catenin-dependent gene transcription and proliferation. We show that cytoneme-based Wnt transport operates in diverse processes, including zebrafish development, the murine intestinal crypt, and human cancer organoids, demonstrating that Wnt transport by cytonemes and its control via the Ror2 pathway is highly conserved in vertebrates.
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Additional details
Related works
- Is cited by
- 10.7554/elife.36953 (DOI)