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Scalable selection of hepatocyte- and hepatocyte precursor-like cells from culture of differentiating transgenically modified murine embryonic stem cells.从转基因修饰的小鼠胚胎干细胞分化培养物中可扩展地选择肝细胞和肝细胞前体样细胞。
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Effects of extracellular matrixes and growth factors on the hepatic differentiation of human embryonic stem cells.细胞外基质和生长因子对人胚胎干细胞肝分化的影响。
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Differentiation of mouse and human embryonic stem cells into hepatic lineages.小鼠和人类胚胎干细胞向肝谱系的分化。
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Hepatic differentiation of mouse embryonic stem cells in a three-dimensional culture system using polyurethane foam.在使用聚氨酯泡沫的三维培养系统中对小鼠胚胎干细胞进行肝向分化。
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Evaluation of HepaRG cells as an in vitro model for human drug metabolism studies.评估HepaRG细胞作为人类药物代谢研究的体外模型。
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Efficient differentiation of hepatocytes from human embryonic stem cells exhibiting markers recapitulating liver development in vivo.从人胚胎干细胞高效分化出的肝细胞表现出在体内重现肝脏发育的标志物。
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使用S-亚硝基乙酰青霉胺从胚胎干细胞中富集具有上调代谢和分化功能的类肝细胞

Enrichment of hepatocyte-like cells with upregulated metabolic and differentiated function derived from embryonic stem cells using S-NitrosoAcetylPenicillamine.

作者信息

Sharma Nripen S, Wallenstein Eric J, Novik Eric, Maguire Tim, Schloss Rene, Yarmush Martin L

机构信息

Department of Chemical and Biochemical Engineering, Rutgers University, Piscataway, New Jersey, USA.

出版信息

Tissue Eng Part C Methods. 2009 Jun;15(2):297-306. doi: 10.1089/ten.tec.2008.0303.

DOI:10.1089/ten.tec.2008.0303
PMID:19196121
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2863155/
Abstract

The generation of a large number of fully functional hepatocytes from a renewable cell source can provide an unlimited resource for bioartificial liver devices and cell replacement therapies. We have established a directed differentiation system using sodium butyrate treatment to generate an enriched population of hepatocyte-like cells from embryonic stem cells. A metabolic analysis of the hepatocyte populations revealed glycolytic and mitochondrial phenotypes similar to mouse hepatoma cells, implying that these cells represent an immature hepatocyte phenotype. To mediate further differentiation, S-NitrosoAcetylPenicillamine (SNAP), a nitric oxide donor, was utilized to induce mitochondrial development in the precursor populations. A comparative analysis of the different treated populations showed that 500microM SNAP treatment resulted in the generation of an enriched population of metabolically mature hepatocyte-like cells with increased differentiated function. Specifically, 500microM SNAP treatment increased glucose consumption, lactate production rates, mitochondrial mass, and potential as compared to untreated populations. In addition, functional analysis revealed that intracellular albumin content, urea secretion rates, and cytochrome P450 7a1 promoter activity were increased in the treated population. The methodology described here to generate an enriched population of metabolically and functionally mature hepatocyte-like cells may have potential implications in drug discovery and regenerative medicine.

摘要

从可再生细胞源生成大量功能齐全的肝细胞可为生物人工肝装置和细胞替代疗法提供无限资源。我们建立了一种使用丁酸钠处理的定向分化系统,以从胚胎干细胞中生成富集的类肝细胞群体。对肝细胞群体的代谢分析揭示了与小鼠肝癌细胞相似的糖酵解和线粒体表型,这意味着这些细胞代表未成熟的肝细胞表型。为了介导进一步分化,使用一氧化氮供体S-亚硝基乙酰青霉胺(SNAP)诱导前体细胞群体中的线粒体发育。对不同处理群体的比较分析表明,500μM SNAP处理导致生成了具有增强分化功能的代谢成熟类肝细胞富集群体。具体而言,与未处理群体相比,500μM SNAP处理提高了葡萄糖消耗、乳酸产生率、线粒体质量和电位。此外,功能分析表明,处理群体中的细胞内白蛋白含量、尿素分泌率和细胞色素P450 7a1启动子活性增加。此处描述的生成代谢和功能成熟类肝细胞富集群体的方法可能在药物发现和再生医学中具有潜在意义。