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Original Genetically modified C3A cells with restored urea cycle for improved bioartificial liver

机译:具有恢复尿素循环的原始转基因C3A细胞,用于改善生物肝脏

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摘要

The bioartificial liver, a hybrid device aimed at improving the survival of patients with fulminant liver failure, requires a cell source to replicate human liver function. However, liver support systems that utilize porcine or human hepatoma-derived cells felt short of expectations in clinical trials. Here we present engineered C3A cells, with a restored function of the urea cycle, which can be used in an efficacious bioartificial liver. The genetic modification was performed using a lentiviral-mediated gene transfer which led to effective integration of the transgenes, coding for arginase I and ornithine transcarbamylase, into the target cell genomes. The engineered cells are more resistant to the oxidative/nitrosative stress induced by the presence of high concentrations of ammonia cations and produce more urea than their unmodified counterparts. Interestingly, the genetically modified cells secrete more albumin than control C3A cells and the synthesis of the protein is induced by increasing concentrations of ammonia. Although the physiological capabilities of the new cell line need to be further examined, at this stage of our study we may conclude that the genetically modified cells are able to convert ammonia to urea more effectively than regular C3A cells. (c) 2020 Nalecz Institute of Biocybernetics and Biomedical Engineering of the Polish Academy of Sciences. Published by Elsevier B.V. All rights reserved.
机译:生物肝脏,一种旨在改善患有膨胀性肝衰竭患者存活的混合装置,需要细胞来源来复制人肝功能。然而,利用猪或人肝癌衍生细胞的肝脏支持系统感到缺乏临床试验的期望。在这里,我们呈现工程化C3A细胞,其尿素循环的恢复功能,可用于有效的生物肝脏。使用慢病毒介导的基因转移进行遗传修饰,其导致转基因的有效整合,编码氨基酶I和鸟氨酸转基氨基甲酰基酶中的靶细胞基因组。工程化细胞对通过高浓度的氨阳离子的存在而诱导的氧化/亚硝基胁迫更耐药,并且产生比未修饰的对应物更多的尿素。有趣的是,通过增加氨浓度诱导蛋白质的遗传修饰的细胞分泌比对照C3A细胞更多的白蛋白分泌更多白蛋白。尽管需要进一步检查新细胞系的生理能力,但在我们研究的这种阶段,我们可以得出结论,转基因细胞能够比常规C3A细胞更有效地将氨转化为尿素。 (c)2020纳尔梁兹生物庭院研究所和波兰科学院生物医学工程。 elsevier b.v出版。保留所有权利。

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