维甲酸
生物
类有机物
再生(生物学)
表型
肠上皮
维甲酸受体
细胞生物学
细胞命运测定
表型筛选
干细胞
细胞分化
遗传异质性
肠粘膜
上皮
遗传学
基因
转录因子
内科学
医学
作者
Ilya Lukonin,Denise Serra,Ludivine Challet Meylan,Katrin Volkmann,Janine Baaten,Rui Zhao,Shelly Meeusen,Karyn Colman,Fabienne Maurer,Michael Stadler,Jeremy L. Jenkins,Prisca Liberali
出处
期刊:Nature
[Springer Nature]
日期:2020-10-07
卷期号:586 (7828): 275-280
被引量:169
标识
DOI:10.1038/s41586-020-2776-9
摘要
The development of intestinal organoids from single adult intestinal stem cells in vitro recapitulates the regenerative capacity of the intestinal epithelium1,2. Here we unravel the mechanisms that orchestrate both organoid formation and the regeneration of intestinal tissue, using an image-based screen to assay an annotated library of compounds. We generate multivariate feature profiles for hundreds of thousands of organoids to quantitatively describe their phenotypic landscape. We then use these phenotypic fingerprints to infer regulatory genetic interactions, establishing a new approach to the mapping of genetic interactions in an emergent system. This allows us to identify genes that regulate cell-fate transitions and maintain the balance between regeneration and homeostasis, unravelling previously unknown roles for several pathways, among them retinoic acid signalling. We then characterize a crucial role for retinoic acid nuclear receptors in controlling exit from the regenerative state and driving enterocyte differentiation. By combining quantitative imaging with RNA sequencing, we show the role of endogenous retinoic acid metabolism in initiating transcriptional programs that guide the cell-fate transitions of intestinal epithelium, and we identify an inhibitor of the retinoid X receptor that improves intestinal regeneration in vivo.
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