Visualization of a short-range Wnt gradient in the intestinal stem-cell niche
- PMID: 26863187
- DOI: 10.1038/nature16937
Visualization of a short-range Wnt gradient in the intestinal stem-cell niche
Abstract
Mammalian Wnt proteins are believed to act as short-range signals, yet have not been previously visualized in vivo. Self-renewal, proliferation and differentiation are coordinated along a putative Wnt gradient in the intestinal crypt. Wnt3 is produced specifically by Paneth cells. Here we have generated an epitope-tagged, functional Wnt3 knock-in allele. Wnt3 covers basolateral membranes of neighbouring stem cells. In intestinal organoids, Wnt3-transfer involves direct contact between Paneth cells and stem cells. Plasma membrane localization requires surface expression of Frizzled receptors, which in turn is regulated by the transmembrane E3 ligases Rnf43/Znrf3 and their antagonists Lgr4-5/R-spondin. By manipulating Wnt3 secretion and by arresting stem-cell proliferation, we demonstrate that Wnt3 mainly travels away from its source in a cell-bound manner through cell division, and not through diffusion. We conclude that stem-cell membranes constitute a reservoir for Wnt proteins, while Frizzled receptor turnover and 'plasma membrane dilution' through cell division shape the epithelial Wnt3 gradient.
Comment in
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Sticking Around: Short-Range Activity of Wnt Ligands.Dev Cell. 2016 Mar 7;36(5):485-6. doi: 10.1016/j.devcel.2016.02.018. Dev Cell. 2016. PMID: 26954543
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Seeing is believing: Wnt3 localization in the gut epithelium.Cell Res. 2016 May;26(5):515-6. doi: 10.1038/cr.2016.41. Epub 2016 Mar 25. Cell Res. 2016. PMID: 27012467 Free PMC article.
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