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Segmented linear modeling of CHO fed-batch culture and its application to large scale production

机译:CHO FED分批文化分段线性建模及其在大规模生产中的应用

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We describe a systematic approach to model CHO metabolism during biopharmaceutical production across a wide range of cell culture conditions. To this end, we applied the metabolic steady state concept. We analyzed and modeled the production rates of metabolites as a function of the specific growth rate. First, the total number of metabolic steady state phases and the location of the breakpoints were determined by recursive partitioning. For this, the smoothed derivative of the metabolic rates with respect to the growth rate were used followed by hierarchical clustering of the obtained partition. We then applied a piecewise regression to the metabolic rates with the previously determined number of phases. This allowed identifying the growth rates at which the cells underwent a metabolic shift. The resulting model with piecewise linear relationships between metabolic rates and the growth rate did well describe cellular metabolism in the fed-batch cultures. Using the model structure and parameter values from a small-scale cell culture (2L) training dataset, it was possible to predict metabolic rates of new fed-batch cultures just using the experimental specific growth rates. Such prediction was successful both at the laboratory scale with 2L bioreactors but also at the production scale of 2000L. This type of modeling provides a flexible framework to set a solid foundation for metabolic flux analysis and mechanistic type of modeling. Biotechnol. Bioeng. 2017;114: 785-797. (c) 2016 The Authors. Biotechnology and Bioengineering Published by Wiley Periodicals, Inc.
机译:我们描述了在各种细胞培养条件下的生物制药过程中模拟Cho新陈代谢的系统方法。为此,我们应用了代谢稳态概念。我们分析并根据特定生长速率的函数进行了分析并建模了代谢物的生产率。首先,通过递归分配确定代谢稳态阶段的总数和断点的位置。为此,使用所获得的分区的分层聚类,使用相对于生长速率的代谢速率的平滑衍生物。然后,我们将分段回归应用于以前确定的阶段的代谢速率。这允许鉴定细胞经历代谢移位的生长速率。由代谢率和生长速率之间的分段线性关系的所得模型对美联储批量培养物描述了细胞代谢。使用来自小规模细胞培养(2L)训练数据集的模型结构和参数值,可以使用实验特异性生长速率来预测新的补料批量培养物的代谢率。这种预测在实验室标度中取得了成功,其中2L生物反应器也在2000L的生产范围内。这种类型的建模提供了一种灵活的框架,用于为代谢通量分析和机械类型的建模设定坚实的框架。 Biotechnol。生物。 2017; 114:785-797。 (c)2016年作者。 Wiley Hearyicals,Inc。出版的生物技术和生物工程

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