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Literature DB >> 29186692

Quiescence Exit of Tert⁺ Stem Cells by Wnt/β-Catenin Is Indispensable for Intestinal Regeneration.

Han Na Suh¹, Moon Jong Kim¹, Youn-Sang Jung¹, Esther M Lien¹, Sohee Jun¹, Jae-Il Park².

Abstract

Fine control of stem cell maintenance and activation is crucial for tissue homeostasis and regeneration. However, the mechanism of quiescence exit of Tert+ intestinal stem cells (ISCs) remains unknown. Employing a Tert knockin (TertTCE/+) mouse model, we found that Tert+ cells are long-term label-retaining self-renewing cells, which are partially distinguished from the previously identified +4 ISCs. Tert+ cells become mitotic upon irradiation (IR) injury. Conditional ablation of Tert+ cells impairs IR-induced intestinal regeneration but not intestinal homeostasis. Upon IR injury, Wnt signaling is specifically activated in Tert+ cells via the ROS-HIFs-transactivated Wnt2b signaling axis. Importantly, conditional knockout of β-catenin/Ctnnb1 in Tert+ cells undermines IR-induced quiescence exit of Tert+ cells, which subsequently impedes intestinal regeneration. Our results that Wnt-signaling-induced activation of Tert+ ISCs is indispensable for intestinal regeneration unveil the underlying mechanism for how Tert+ stem cells undergo quiescence exit upon tissue injury.

Entities: CellLine Chemical Disease Gene Mutation Species

Keywords: ROS-HIFs-Wnt2b; Tert; Wnt/β-catenin; intestinal regeneration; intestinal stem cells; radiation

Mesh：

Substances：

Year: 2017 PMID： 29186692 PMCID： PMC5726811 DOI： 10.1016/j.celrep.2017.10.118

Source DB: PubMed Journal: Cell Rep Impact factor: 9.423

44 in total

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