生物
类有机物
诱导多能干细胞
干细胞
细胞生物学
体内
癌症研究
胚胎干细胞
生物技术
遗传学
基因
作者
Holly M. Poling,Nambirajan Sundaram,Garrett W. Fisher,Akaljot Singh,Joseph R Shiley,Kalpana Nattamai,Vinothini Govindarajah,Alexander R. Cortez,Maksym Krutko,Séverine Ménoret,Ignacio Anegón,Magdalena Kasendra,James M. Wells,Christopher N. Mayhew,Takanori Takebe,Maxime M. Mahé,Michael A. Helmrath
标识
DOI:10.1016/j.stem.2024.08.009
摘要
The fundamental goal of tissue engineering is to functionally restore or improve damaged tissues or organs. Here we address this in the small bowel using an in vivo xenograft preclinical acute damage model. We investigated the therapeutic capacity of human intestinal organoids (HIOs), which are generated from human pluripotent stem cells (hPSCs), to repair damaged small bowel. We hypothesized that the HIO's cellular complexity would allow it to sustain transmural engraftment. To test this, we developed a rodent injury model where, through luminal delivery, we demonstrated that fragmented HIOs engraft, proliferate, and persist throughout the bowel following repair. Not only was restitution of the mucosal layer observed, but significant incorporation was also observed in the muscularis and vascular endothelium. Further analysis characterized sustained cell type presence within the regenerated regions, retention of proximal regionalization, and the neo-epithelia's function. These findings demonstrate the therapeutic importance of mesenchyme for intestinal injury repair.
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