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三维 HepaRG 模型作为一种有吸引力的毒性测试工具。

Three-dimensional HepaRG model as an attractive tool for toxicity testing.

机构信息

Instituto de Biologia Experimental e Tecnológica, 2781-901 Oeiras, Portugal.

出版信息

Toxicol Sci. 2012 Nov;130(1):106-16. doi: 10.1093/toxsci/kfs232. Epub 2012 Jul 27.

Abstract

The culture of HepaRG cells as three dimensional (3D) structures in the spinner-bioreactor may represent added value as a hepatic system for toxicological purposes. The use of a cost-effective commercially available bioreactor, which is compatible with high-throughput cell analysis, constitutes an attractive approach for routine use in the drug testing industry. In order to assess specific aspects of the biotransformation capacity of the bioreactor-based HepaRG system, the induction of CYP450 enzymes (i.e., CYP1A2, 2B6, 2C9, and 3A4) and the activity of the phase II enzyme, uridine diphosphate glucuronoltransferase (UGT), were tested. The long-term functionality of the system was demonstrated by 7-week stable profiles of albumin secretion, CYP3A4 induction, and UGT activities. Immunofluorescence-based staining showed formation of tissue-like arrangements including bile canaliculi-like structures and polar distribution of transporters. The use of in silico models to analyze the in vitro data related to hepatotoxic activity of acetaminophen (APAP) demonstrated the advantage of the integration of kinetic and dynamic aspects for a better understanding of the in vitro cell behavior. The bioactivation of APAP and its related cytotoxicity was assessed in a system compatible to high-throughput screening. The approach also proved to be a good strategy to reduce the time necessary to obtain fully differentiated cell cultures. In conclusion, HepaRG cells cultured in 3D spinner-bioreactors are an attractive tool for toxicological studies, showing a liver-like performance and demonstrating a practical applicability for toxicodynamic approaches.

摘要

在旋转生物反应器中培养的三维(3D)HepaRG 细胞可能代表了一种具有附加值的肝系统,可用于毒理学目的。使用经济高效的市售生物反应器,该生物反应器与高通量细胞分析兼容,是药物测试行业常规使用的有吸引力的方法。为了评估基于生物反应器的 HepaRG 系统的生物转化能力的特定方面,测试了 CYP450 酶(即 CYP1A2、2B6、2C9 和 3A4)的诱导和相 II 酶尿苷二磷酸葡萄糖醛酸基转移酶 (UGT) 的活性。该系统的长期功能通过 7 周稳定的白蛋白分泌、CYP3A4 诱导和 UGT 活性的曲线得到证明。基于免疫荧光的染色显示了组织样排列的形成,包括胆小管样结构和转运蛋白的极性分布。使用计算模型分析与对乙酰氨基酚 (APAP) 的肝毒性活性相关的体外数据表明,整合动力学和动态方面的优势对于更好地理解体外细胞行为是有利的。在与高通量筛选兼容的系统中评估了 APAP 的生物活化及其相关的细胞毒性。该方法还被证明是减少获得完全分化细胞培养所需时间的良好策略。总之,在 3D 旋转生物反应器中培养的 HepaRG 细胞是毒理学研究的一种有吸引力的工具,表现出类肝性能,并证明了用于毒动学方法的实际适用性。

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