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鼠胎儿肠类器官:研究从哺乳期到离乳期上皮成熟的新模型。

Mouse fetal intestinal organoids: new model to study epithelial maturation from suckling to weaning.

机构信息

Department of Gastroenterology and Hepatology, Tytgat Institute for Liver and Intestinal Research, Amsterdam UMC, AG&M, University of Amsterdam, Amsterdam, The Netherlands.

Department of Pediatrics, Amsterdam UMC, University of Amsterdam, Amsterdam, The Netherlands.

出版信息

EMBO Rep. 2019 Feb;20(2). doi: 10.15252/embr.201846221. Epub 2018 Dec 10.

Abstract

During the suckling-to-weaning transition, the intestinal epithelium matures, allowing digestion of solid food. Transplantation experiments with rodent fetal epithelium into subcutaneous tissue of adult animals suggest that this transition is intrinsically programmed and occurs in the absence of dietary or hormonal signals. Here, we show that organoids derived from mouse primary fetal intestinal epithelial cells express markers of late fetal and neonatal development. In a stable culture medium, these fetal epithelium-derived organoids lose all markers of neonatal epithelium and start expressing hallmarks of adult epithelium in a time frame that mirrors epithelial maturation postnatal development of the fetal-derived organoids accelerates by dexamethasone, a drug used to accelerate intestinal maturation Together, our data show that organoids derived from fetal epithelium undergo suckling-to-weaning transition, that the speed of maturation can be modulated, and that fetal organoids can be used to model the molecular mechanisms of postnatal epithelial maturation.

摘要

在哺乳到断奶的过渡期间,肠上皮成熟,允许消化固体食物。用啮齿动物胎儿上皮细胞移植到成年动物的皮下组织的实验表明,这种转变是内在程序化的,并且在没有饮食或激素信号的情况下发生。在这里,我们表明,源自小鼠原代胎儿肠上皮细胞的类器官表达晚期胎儿和新生儿发育的标志物。在稳定的培养基中,这些胎儿上皮衍生的类器官失去所有新生儿上皮的标志物,并开始表达成年上皮的特征,其时间框架与胎儿衍生类器官的上皮成熟后发育相吻合。地塞米松可加速类器官的成熟,一种用于加速肠成熟的药物。总之,我们的数据表明,源自胎儿上皮的类器官经历了哺乳到断奶的过渡,成熟的速度可以调节,并且胎儿类器官可用于模拟出生后上皮成熟的分子机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f06d/6362357/9e00ef50176c/EMBR-20-e46221-g002.jpg

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