Partial in vivo reprogramming enables injury-free intestinal regeneration via autonomous Ptgs1 induction

体内部分重编程可通过自主诱导Ptgs1实现无损伤的肠道再生。

阅读:5
作者:Jumee Kim ,Somi Kim ,Seung-Yeon Lee ,Beom-Ki Jo ,Ji-Young Oh ,Eun-Ji Kwon ,Keun-Tae Kim ,Anish Ashok Adpaikar ,Eun-Jung Kim ,Han-Sung Jung ,Hwa-Ryeon Kim ,Jae-Seok Roe ,Chang Pyo Hong ,Jong Kyoung Kim ,Bon-Kyoung Koo ,Hyuk-Jin Cha
期刊:Science Advances影响因子:11.700
时间:2023起止号:2023 Nov 24;9(47):eadi8454.
doi:10.1126/sciadv.adi8454方法学: FCM、IF、IHC-P
研究方向: 信号转导

Abstract

Tissue regeneration after injury involves the dedifferentiation of somatic cells, a natural adaptive reprogramming that leads to the emergence of injury-responsive cells with fetal-like characteristics. However, there is no direct evidence that adaptive reprogramming involves a shared molecular mechanism with direct cellular reprogramming. Here, we induced dedifferentiation of intestinal epithelial cells using OSKM (Oct4, Sox2, Klf4, and c-Myc) in vivo. The OSKM-induced forced dedifferentiation showed similar molecular features of intestinal regeneration, including a transition from homeostatic cell types to injury-responsive-like cell types. These injury-responsive-like cells, sharing gene signatures of revival stem cells and atrophy-induced villus epithelial cells, actively assisted tissue regeneration following damage. In contrast to normal intestinal regeneration involving Ptgs2 induction, the OSKM promotes autonomous production of prostaglandin E2 via epithelial Ptgs1 expression. These results indicate prostaglandin synthesis is a common mechanism for intestinal regeneration but involves a different enzyme when partial reprogramming is applied to the intestinal epithelium.

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