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Villification in the mouse: Bmp signals control intestinal villus patterning

dc.contributor.authorWalton, KD
dc.contributor.authorWhidden, M
dc.contributor.authorKolterud, Å
dc.contributor.authorShoffner, SK
dc.contributor.authorCzerwinski, MJ
dc.contributor.authorKushwaha, J
dc.contributor.authorParmar, N
dc.contributor.authorChandhrasekhar, D
dc.contributor.authorFreddo, AM
dc.contributor.authorSchnell, S
dc.contributor.authorGumucio, DL
dc.coverage.spatialEngland
dc.date.accessioned2023-01-09T17:56:22Z
dc.date.available2023-01-09T17:56:22Z
dc.date.issued2016-02-01
dc.identifier.issn0950-1991
dc.identifier.issn1477-9129
dc.identifier.urihttps://www.ncbi.nlm.nih.gov/pubmed/26721501
dc.identifier.urihttps://hdl.handle.net/2027.42/175370en
dc.description.abstractIn the intestine, finger-like villi provide abundant surface area for nutrient absorption. During murine villus development, epithelial Hedgehog (Hh) signals promote aggregation of subepithelial mesenchymal clusters that drive villus emergence. Clusters arise first dorsally and proximally and spread over the entire intestine within 24 h, but the mechanism driving this pattern in the murine intestine is unknown. In chick, the driver of cluster pattern is tensile force from developing smooth muscle, which generates deep longitudinal epithelial folds that locally concentrate the Hh signal, promoting localized expression of cluster genes. By contrast, we show that in mouse, muscle-induced epithelial folding does not occur and artificial deformation of the epithelium does not determine the pattern of clusters or villi. In intestinal explants, modulation of Bmp signaling alters the spatial distribution of clusters and changes the pattern of emerging villi. Increasing Bmp signaling abolishes cluster formation, whereas inhibiting Bmp signaling leads to merged clusters. These dynamic changes in cluster pattern are faithfully simulated by a mathematical model of a Turing field in which an inhibitor of Bmp signaling acts as the Turing activator. In vivo, genetic interruption of Bmp signal reception in either epithelium or mesenchyme reveals that Bmp signaling in Hh-responsive mesenchymal cells controls cluster pattern. Thus, unlike in chick, the murine villus patterning system is independent of muscle-induced epithelial deformation. Rather, a complex cocktail of Bmps and Bmp signal modulators secreted from mesenchymal clusters determines the pattern of villi in a manner that mimics the spread of a self-organizing Turing field.
dc.format.mediumPrint-Electronic
dc.languageeng
dc.publisherThe Company of Biologists
dc.subjectActivator-inhibitor patterning model
dc.subjectEpithelial-mesenchymal crosstalk
dc.subjectIntestinal development
dc.subjectMathematical model
dc.subjectMorphogenesis
dc.subjectTuring field
dc.subjectVillus formation
dc.subjectAnimals
dc.subjectBody Patterning
dc.subjectBone Morphogenetic Protein Receptors, Type I
dc.subjectBone Morphogenetic Proteins
dc.subjectEpithelium
dc.subjectHedgehog Proteins
dc.subjectIn Situ Hybridization
dc.subjectIntestines
dc.subjectLigands
dc.subjectMesoderm
dc.subjectMice, Inbred C57BL
dc.subjectMicrovilli
dc.subjectModels, Biological
dc.subjectMuscle, Smooth
dc.subjectOrgan Size
dc.subjectSignal Transduction
dc.subjectTensile Strength
dc.titleVillification in the mouse: Bmp signals control intestinal villus patterning
dc.typeArticle
dc.identifier.pmid26721501
dc.description.bitstreamurlhttp://deepblue.lib.umich.edu/bitstream/2027.42/175370/2/DownloadCombinedArticleAndSupplmentPdf.pdf
dc.identifier.doi10.1242/dev.130112
dc.identifier.doihttps://dx.doi.org/10.7302/6751
dc.identifier.sourceDevelopment (Cambridge)
dc.description.versionPublished version
dc.date.updated2023-01-09T17:56:19Z
dc.identifier.orcid0000-0001-9108-5617
dc.identifier.orcid0000-0002-9477-3914
dc.description.filedescriptionDescription of DownloadCombinedArticleAndSupplmentPdf.pdf : Published version
dc.identifier.volume143
dc.identifier.issue3
dc.identifier.startpage427
dc.identifier.endpage436
dc.identifier.name-orcidWalton, KD; 0000-0001-9108-5617
dc.identifier.name-orcidWhidden, M
dc.identifier.name-orcidKolterud, Å
dc.identifier.name-orcidShoffner, SK
dc.identifier.name-orcidCzerwinski, MJ
dc.identifier.name-orcidKushwaha, J
dc.identifier.name-orcidParmar, N
dc.identifier.name-orcidChandhrasekhar, D
dc.identifier.name-orcidFreddo, AM
dc.identifier.name-orcidSchnell, S; 0000-0002-9477-3914
dc.identifier.name-orcidGumucio, DL
dc.working.doi10.7302/6751en
dc.owningcollnameInternal Medicine, Department of


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