首页> 外文期刊>Tissue engineering, Part A >Three-dimensional perfusion bioreactor culture supports differentiation of human fetal liver cells.
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Three-dimensional perfusion bioreactor culture supports differentiation of human fetal liver cells.

机译:三维灌注生物反应器培养支持人胎儿肝细胞的分化。

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The ability of human fetal liver cells to survive, expand, and form functional tissue in vitro is of high interest for the development of bioartificial extracorporeal liver support systems, liver cell transplantation therapies, and pharmacologic models. Conventional static two-dimensional culture models seem to be inadequate tools. We focus on dynamic three-dimensional perfusion technologies and developed a scaled-down bioreactor, providing decentralized mass exchange with integral oxygenation. Human fetal liver cells were embedded in a hyaluronan hydrogel within the capillary system to mimic an in vivo matrix and perfusion environment. Metabolic performance was monitored daily, including glucose consumption, lactate dehydrogenase activity, and secretion of alpha-fetoprotein and albumin. At culture termination cells were analyzed for proliferation and liver-specific lineage-dependent cytochrome P450 (CYP3A4/3A7) gene expression. Occurrence of hepatic differentiation in bioreactor cultures was demonstrated by a strong increase in CYP3A4/3A7 gene expression ratio, lower alpha-fetoprotein, and higher albumin secretion than in conventional Petri dish controls. Cells in bioreactors formed three-dimensional structures. Viability of cells was higher in bioreactors than in control cultures. In conclusion, the culture model implementing three-dimensionality, constant perfusion, and integral oxygenation in combination with a hyaluronan hydrogel provides superior conditions for liver cell survival and differentiation compared to conventional culture.
机译:人类胎儿肝细胞在体外存活,扩增和形成功能性组织的能力对于生物人工体外肝支持系统,肝细胞移植疗法和药理模型的开发非常感兴趣。传统的静态二维文化模型似乎不足以作为工具。我们专注于动态三维灌注技术,并开发了按比例缩小的生物反应器,可通过整体充氧提供分散的质量交换。将人类胎儿肝细胞嵌入毛细管系统内的透明质酸水凝胶中,以模拟体内基质和灌注环境。每天监测代谢性能,包括葡萄糖消耗,乳酸脱氢酶活性以及甲胎蛋白和白蛋白的分泌。在培养终止时,分析细胞的增殖和肝特异性谱系依赖性细胞色素P450(CYP3A4 / 3A7)基因表达。与常规培养皿对照相比,CYP3A4 / 3A7基因表达比例的强烈增加,较低的甲胎蛋白和较高的白蛋白分泌证明了生物反应器培养物中肝细胞分化的发生。生物反应器中的细胞形成三维结构。生物反应器中的细胞活力高于对照培养物中的细胞活力。总之,与透明质酸培养相比,结合三维透明质酸水凝胶实现三维,恒定灌注和整体氧合的培养模型为肝细胞存活和分化提供了优越的条件。

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