原代肝细胞包裹聚集体在填充床生物反应器中的培养:一种潜在的生物人工肝。

A P Li, G Barker, D Beck, S Colburn, R Monsell, C Pellegrin
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引用次数: 19

摘要

传统的肝细胞培养系统通常包括在静态培养基池中培养成扁平单层细胞的细胞,细胞间接触有限,不像活体肝脏,实质细胞是立方体的,细胞间接触广泛,并且持续灌注血液。我们在此报告了一种新的生物反应器系统,用于培养具有立方体细胞形状,广泛细胞间接触和灌注介质的原代肝细胞。将肝细胞接种到生物反应器中,并使其以最佳速率再循环,使其碰撞并形成聚集体。这些新形成的聚集体随后被困在玻璃珠堆积的床中。生物反应器灌注含氧营养培养基,控制氧张力、pH和培养基灌注率。根据尿素合成、白蛋白合成和细胞形态,肝细胞在培养中存活最长时间为15天。在生物反应器中培养15天的肝细胞光镜研究显示,肝器官中有类似肝细胞板的相互连接的三维结构。电镜观察显示其超微结构与体内肝细胞相似,包括存在丰富的线粒体、粗糙光滑的内质网、糖原颗粒、过氧化物酶体和桥粒。我们相信我们的肝细胞生物反应器是对传统培养系统的重大改进,具有重要的工业应用,包括毒理学,药物代谢和蛋白质/肽合成。肝细胞生物反应器的概念也可以作为发展生物人工肝的基础,为肝功能衰竭患者提供体外肝支持。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Culturing of primary hepatocytes as entrapped aggregates in a packed bed bioreactor: a potential bioartificial liver.

Conventional culture systems for hepatocytes generally involve cells cultured as flat, monolayer cells, with limited cell-cell contact, in a static pool of medium, unlike the liver in vivo where the parenchymal cells are cuboidal, with extensive cell-cell contact, and are continuously perfused with blood. We report here a novel bioreactor system for the culturing of primary hepatocytes with cuboidal cell shape, extensive cell-cell contact, and perfusing medium. The hepatocytes were inoculated into the bioreactor and allowed to recirculate at a rate optimal for them to collide and form aggregates. These newly-formed aggregates were subsequently entrapped in a packed bed of glass beads. The bioreactor was perfused with oxygenated nutrient medium, with controlled oxygen tension, pH, and medium perfusion rate. The hepatocytes were viable for up to the longest time point studied of 15 days in culture based on urea synthesis, albumin synthesis and cell morphology. Light microscopy studies of hepatocytes cultured for 15 days in the bioreactor showed interconnecting three-dimensional structures resembling the hepatic cell plate in the liver organ. Electron microscopy studies on the same cells revealed ultrastructure similar to the hepatocytes in vivo, including the presence of plentiful mitochondria, rough and smooth endoplasmic reticulum, glycogen granules, peroxisomes, and desmosomes. We believe that our hepatocyte bioreactor is a major improvement over conventional culture systems, with important industrial applications including toxicology, drug metabolism, and protein/peptide synthesis. The hepatocyte bioreactor concept may also be used as the basis for the development of a bioartificial liver to provide extracorporeal hepatic support to patients with hepatic failure.

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