Establishment of intestinal organoid cultures modeling injury-associated epithelial regeneration

类有机物 生物 再生(生物学) LGR5型 重编程 干细胞 细胞生物学 表观基因组 再生医学 细胞 癌症干细胞 DNA甲基化 遗传学 基因 基因表达
作者
Molong Qu,Liang Xiong,Yulin Lyu,Xiannian Zhang,J. Shen,Jingyang Guan,Peiyuan Chai,Zhongqing Lin,Boyao Nie,Cheng Li,Jun Xu,Hongkui Deng
出处
期刊:Cell Research [Springer Nature]
卷期号:31 (3): 259-271 被引量:100
标识
DOI:10.1038/s41422-020-00453-x
摘要

Abstract The capacity of 3D organoids to mimic physiological tissue organization and functionality has provided an invaluable tool to model development and disease in vitro. However, conventional organoid cultures primarily represent the homeostasis of self-organizing stem cells and their derivatives. Here, we established a novel intestinal organoid culture system composed of 8 components, mainly including VPA, EPZ6438, LDN193189, and R-Spondin 1 conditioned medium, which mimics the gut epithelium regeneration that produces hyperplastic crypts following injury; therefore, these organoids were designated hyperplastic intestinal organoids (Hyper-organoids). Single-cell RNA sequencing identified different regenerative stem cell populations in our Hyper-organoids that shared molecular features with in vivo injury-responsive Lgr5 + stem cells or Clu + revival stem cells. Further analysis revealed that VPA and EPZ6438 were indispensable for epigenome reprogramming and regeneration in Hyper-organoids, which functioned through epigenetically regulating YAP signaling. Furthermore, VPA and EPZ6438 synergistically promoted regenerative response in gut upon damage in vivo. In summary, our results demonstrated a new in vitro organoid model to study epithelial regeneration, highlighting the importance of epigenetic reprogramming that pioneers tissue repair.
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