Mini-gut organoids: reconstitution of the stem cell niche.

Date S; Sato T

doi:10.1146/annurev-cellbio-100814-125218

Mini-gut organoids: reconstitution of the stem cell niche.

Date S ¹,

Sato T ¹

Affiliations

1. Department of Gastroenterology, Keio University School of Medicine, Tokyo 108-8345, Japan;
Authors
Date S¹
Sato T¹
(2 authors)

ORCIDs linked to this article

Sato T | 0000-0001-8353-8137

Annual Review of Cell and Developmental Biology, 02 Oct 2015, 31:269-289
https://doi.org/10.1146/annurev-cellbio-100814-125218 PMID: 26436704

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Abstract

In the adult mammalian body, self-renewal of tissue stem cells is regulated by extracellular niche environments in response to the demands of tissue organization. Intestinal stem cells expressing Lgr5 constantly self-renew in their specific niche at the crypt bottom to maintain rapid turnover of the epithelium. Niche-regulated stem cell self-renewal is perturbed in several mouse genetic models and during human tumorigenesis, suggesting roles for EGF, Wnt, BMP/TGF-β, and Notch signaling. In vitro niche reconstitution capitalizing on this knowledge has enabled the growth of single intestinal stem cells into mini-gut epithelial organoids comprising Lgr5(+) stem cells and all types of differentiated lineages. The mini-gut organoid culture platform is applicable to various types of digestive tissue epithelium from multiple species. The mechanism of self-renewal in organoids provides novel insights for organogenesis, regenerative medicine, and tumorigenesis of the digestive system.

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Read article at publisher's site: https://doi.org/10.1146/annurev-cellbio-100814-125218

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Search life-sciences literature (45,103,589 articles, preprints and more)

Mini-gut organoids: reconstitution of the stem cell niche.

Affiliations

Authors

ORCIDs linked to this article

Abstract

Full text links

References

Morphological observations on mucus-secreting nongoblet cells in the deep crypts of the rat ascending colon.

Adult intestinal stem cells: critical drivers of epithelial homeostasis and regeneration.

Lgr5(+ve) stem cells drive self-renewal in the stomach and build long-lived gastric units in vitro.

Identification of stem cells in small intestine and colon by marker gene Lgr5.

In vitro expansion of human gastric epithelial stem cells and their responses to bacterial infection.

Clonal analysis of mouse intestinal epithelial progenitors.

Intestinal epithelial stem cells and progenitors.

Self-renewal, multipotency, and the existence of two cell populations within an epithelial stem cell niche.

Organoid models of human and mouse ductal pancreatic cancer.

Intestinal label-retaining cells are secretory precursors expressing Lgr5.

Citations & impact

Impact metrics

Citations of article over time

Alternative metrics

Article citations

The Future Exploring of Gut Microbiome-Immunity Interactions: From In Vivo/Vitro Models to In Silico Innovations.

Ontogeny of Skin Stem Cells and Molecular Underpinnings.

Isolation of Myenteric and Submucosal Plexus from Mouse Gastrointestinal Tract and Subsequent Co-Culture with Small Intestinal Organoids.

Advances in the Study of Common and Rare CFTR Complex Alleles Using Intestinal Organoids.

Repurposing Metabolic Inhibitors in the Treatment of Colon Adenocarcinoma Patient-Derived Models.

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Mini-gut organoids: reconstitution of the stem cell niche.

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