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A Rational Design Approach for Amino Acid Supplementation in Hepatocyte Culture

机译:肝细胞培养中氨基酸补充的合理设计方法

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Improvement of culture media for mammalian cells is conducted via empirical adjustments, sometimes aided by statistical design methodologies. Here, we demonstrate a proof of principle for the use of constraints-based modeling to achieve enhanced performance of liver-specific functions of cultured hepatocytes during plasma exposure by adjusting amino acid supplementation and hormone levels in the medium. Flux balance analysis (FBA) is used to determine an amino acid flux profile consistent with a desired output; this is used to design an amino acid supplementation. Under conditions of no supplementation, empirical supplementation, and designed supplementation, hepatocytes were exposed to plasma and their morphology, specific cell functions (urea, albumin production) and lipid metabolism were measured. Urea production under the designed amino acid supplementation was found to be increased compared with previously reported (empirical) amino acid supplementation. Not surprisingly, the urea production attained was less than the theoretical value, indicating the existence of pathways or constraints not present in, the current model. Although not an explicit design objective, albumin production was also increased by designed amino acid supplementation, suggesting a functional linkage between these outputs. In conjunction with traditional approaches to improving culture conditions, the rational design approach described herein provides a novel means to tune the metabolic outputs of cultured hepatocytes. Biotechnol. Bioeng. 2009;103: 1176-1191.
机译:哺乳动物细胞培养基的改良是通过经验调整进行的,有时可以通过统计设计方法进行辅助。在这里,我们演示了使用基于约束的建模来通过调整培养基中的氨基酸补充和激素水平来提高血浆暴露期间培养的肝细胞肝特异性功能的性能的原理证明。助焊剂平衡分析(FBA)用于确定与所需输出一致的氨基酸通量图;这用于设计氨基酸补充。在不进行补充,经验性补充和设计性补充的条件下,将肝细胞暴露于血浆中,并测量其形态,特定细胞功能(尿素,白蛋白生成)和脂质代谢。发现与先前报道的(经验)氨基酸补充相比,在设计氨基酸补充下的尿素生产增加了。毫不奇怪,所获得的尿素产量低于理论值,表明存在当前模型中不存在的途径或约束。尽管这不是一个明确的设计目标,但通过设计氨基酸的补充,白蛋白的产量也增加了,这表明这些输出之间存在功能联系。结合改善培养条件的传统方法,本文所述的合理设计方法提供了一种新颖的手段来调节培养的肝细胞的代谢输出。生物技术。生恩2009; 103:1176-1191。

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