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METHODS AND SYSTEMS FOR CONVERTING PRECURSOR CELLS INTO INTESTINAL TISSUES THROUGH DIRECTED DIFFERENTIATION

机译:通过定向分化将前体细胞转化为肠组织的方法和系统

摘要

The generation of complex organ tissues from human embryonic and pluripotent stem cells (PSCs) remains a major challenge for translational studies. It is shown that PSCs can be directed to differentiate into intestinal tissue in vitro by modulating the combinatorial activities of several signaling pathways in a step-wise fashion, effectively recapitulating in vivo fetal intestinal development. The resulting intestinal “organoids” were three-dimensional structures consisting of a polarized, columnar epithelium surrounded by mesenchyme that included a smooth muscle-like layer. The epithelium was patterned into crypt-like SOX9-positive proliferative zones and villus-like structures with all of the major functional cell types of the intestine. The culture system is used to demonstrate that expression of NEUROG3, a pro-endocrine transcription factor mutated in enteric anendocrinosis is sufficient to promote differentiation towards the enteroendocrine cell lineage. In conclusion, PSC-derived human intestinal tissue should allow for unprecedented studies of human intestinal development, homeostasis and disease.
机译:从人类胚胎和多能干细胞(PSC)产生复杂器官组织仍然是翻译研究的主要挑战。结果表明,通过逐步调节几种信号传导途径的组合活性,可以有效地概括体内胎儿肠道的发育,从而指导PSCs在体外分化为肠道组织。最终的肠道“类器官”是三维结构,由极化,柱状上皮和间质包围,其中包括平滑肌样层。上皮被图案化为具有肠所有主要功能细胞类型的隐窝样SOX9阳性增生区和绒毛样结构。该培养系统用于证明NEUROG3(一种在肠内分泌中突变的内分泌前转录因子)的表达足以促进其向肠内分泌细胞谱系的分化。总之,PSC衍生的人类肠道组织应允许对人类肠道发育,体内稳态和疾病进行前所未有的研究。

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