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Barrier Properties and Transcriptome Expression in Human iPSC-Derived Models of the Blood-Brain Barrier

机译:血脑屏障人体IPSC衍生模型中的阻隔性和转录组表达

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Cell-based models of the blood-brain barrier (BBB) are important for increasing the knowledge of BBB formation, degradation and brain exposure of drug substances. Human models are preferred over animal models because of interspecies differences in BBB structure and function. However, access to human primary BBB tissue is limited and has shown degeneration of BBB functions in vitro. Human induced pluripotent stem cells (iPSCs) can be used to generate relevant cell types to model the BBB with human tissue. We generated a human iPSC-derived model of the BBB that includes endothelial cells in coculture with pericytes, astrocytes and neurons. Evaluation of barrier properties showed that the endothelial cells in our coculture model have high transendothelial electrical resistance, functional efflux and ability to discriminate between CNS permeable and non-permeable substances. Whole genome expression profiling revealed transcriptional changes that occur in coculture, including upregulation of tight junction proteins, such as claudins and neurotransmitter transporters. Pathway analysis implicated changes in the WNT, TNF, and PI3K-Akt pathways upon coculture. Our data suggest that coculture of iPSC-derived endothelial cells promotes barrier formation on a functional and transcriptional level. The information about gene expression changes in coculture can be used to further improve iPSC-derived BBB models through selective pathway manipulation.
机译:基于细胞的血脑屏障模型(BBB)对于增加BBB形成,降解和药物脑暴露的知识是重要的。由于BBB结构和功能的差异,人类模型优于动物模型。然而,对人的原发性BBB组织有限,并且已经在体外显示了BBB功能的退化。人诱导多能干细胞(IPSC)可用于产生相关细胞类型以将BBB与人体组织进行模拟。我们生成了BBB的人类IPSC衍生模型,其包括与细胞,星形胶质细胞和神经元共培养的内皮细胞。屏障性质的评价表明,我们的共培育模型中的内皮细胞具有高的经胸壁电阻,功能性渗透性和区分CNS可渗透和不渗透物质的能力。全基因组表达分析揭示了共培养物中发生的转录变化,包括狭窄结蛋白的上调,例如克劳德林和神经递质转运蛋白。途径分析意义在共培养时WNT,TNF和PI3K-AKT路径的变化。我们的数据表明,IPSC衍生的内皮细胞的共培养促进了功能性和转录水平的屏障形成。通过选择性途径操纵,可以使用有关共培养基因表达变化的信息的信息来进一步改进IPSC导出的BBB模型。

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