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Publication : Smooth muscle contributes to the development and function of a layered intestinal stem cell niche.

First Author  McCarthy N Year  2023
Journal  Dev Cell Volume  58
Issue  7 Pages  550-564.e6
PubMed ID  36924771 Mgi Jnum  J:352456
Mgi Id  MGI:7463869 Doi  10.1016/j.devcel.2023.02.012
Citation  McCarthy N, et al. (2023) Smooth muscle contributes to the development and function of a layered intestinal stem cell niche. Dev Cell 58(7):550-564.e6
abstractText  Wnt and Rspondin (RSPO) signaling drives proliferation, and bone morphogenetic protein inhibitors (BMPi) impede differentiation, of intestinal stem cells (ISCs). Here, we identify the mouse ISC niche as a complex, multi-layered structure that encompasses distinct mesenchymal and smooth muscle populations. In young and adult mice, diverse sub-cryptal cells provide redundant ISC-supportive factors; few of these are restricted to single cell types. Niche functions refine during postnatal crypt morphogenesis, in part to oppose the dense aggregation of differentiation-promoting BMP+ sub-epithelial myofibroblasts at crypt-villus junctions. Muscularis mucosae, a specialized muscle layer, first appears during this period and supplements neighboring RSPO and BMPi sources. Components of this developing niche are conserved in human fetuses. The in vivo ablation of mouse postnatal smooth muscle increases BMP signaling activity, potently limiting a pre-weaning burst of crypt fission. Thus, distinct and progressively specialized mesenchymal cells together create the milieu that is required to propagate crypts during rapid organ growth and to sustain adult ISCs.
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