4.7 Article

Stroma provides an intestinal stem cell niche in the absence of epithelial Wnts

期刊

DEVELOPMENT
卷 141, 期 11, 页码 2206-2215

出版社

COMPANY BIOLOGISTS LTD
DOI: 10.1242/dev.104976

关键词

Wnt; PORCN; Radiation injury; R-spondin; Intestinal niche; Mouse

资金

  1. National Research Foundation Singapore under its STAR Award Program
  2. A*STAR Translational Clinical Research Partnership grant
  3. March of Dimes Foundation [6-FY08-315]

向作者/读者索取更多资源

Wnt/beta-catenin signaling supports intestinal homeostasis by regulating proliferation in the crypt. Multiple Wnts are expressed in Paneth cells as well as other intestinal epithelial and stromal cells. Ex vivo, Wnts secreted by Paneth cells can support intestinal stem cells when Wnt signaling is enhanced with supplemental R-Spondin 1 (RSPO1). However, in vivo, the source of Wnts in the stem cell niche is less clear. Genetic ablation of Porcn, an endoplasmic reticulum resident O-acyltransferase that is essential for the secretion and activity of all vertebrate Wnts, confirmed the role of intestinal epithelial Wnts in ex vivo culture. Unexpectedly, mice lacking epithelial Wnt activity (Porcn(Del)/Villin-Cre mice) had normal intestinal proliferation and differentiation, as well as successful regeneration after radiation injury, indicating that epithelial Wnts are dispensable for these processes. Consistent with a key role for stroma in the crypt niche, intestinal stromal cells endogenously expressing Wnts and Rspo3 support the growth of Porcn(Del) organoids ex vivo without RSPO1 supplementation. Conversely, increasing pharmacologic PORCN inhibition, affecting both stroma and epithelium, reduced Lgr5 intestinal stem cells, inhibited recovery from radiation injury, and at the highest dose fully blocked intestinal proliferation. We conclude that epithelial Wnts are dispensable and that stromal production of Wnts can fully support normal murine intestinal homeostasis.

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