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混合基本通量分析/非参数建模:在生物过程控制中的应用

Hybrid elementary flux analysis/nonparametric modeling: application for bioprocess control.

作者信息

Teixeira Ana P, Alves Carlos, Alves Paula M, Carrondo Manuel J T, Oliveira Rui

机构信息

IBET/ITQB, Apartado 12, P-2781-901 Oeiras, Portugal.

出版信息

BMC Bioinformatics. 2007 Jan 29;8:30. doi: 10.1186/1471-2105-8-30.

Abstract

BACKGROUND

The progress in the "-omic" sciences has allowed a deeper knowledge on many biological systems with industrial interest. This knowledge is still rarely used for advanced bioprocess monitoring and control at the bioreactor level. In this work, a bioprocess control method is presented, which is designed on the basis of the metabolic network of the organism under consideration. The bioprocess dynamics are formulated using hybrid rigorous/data driven systems and its inherent structure is defined by the metabolism elementary modes.

RESULTS

The metabolic network of the system under study is decomposed into elementary modes (EMs), which are the simplest paths able to operate coherently in steady-state. A reduced reaction mechanism in the form of simplified reactions connecting substrates with end-products is obtained. A dynamical hybrid system integrating material balance equations, EMs reactions stoichiometry and kinetics was formulated. EMs kinetics were defined as the product of two terms: a mechanistic/empirical known term and an unknown term that must be identified from data, in a process optimisation perspective. This approach allows the quantification of fluxes carried by individual elementary modes which is of great help to identify dominant pathways as a function of environmental conditions. The methodology was employed to analyse experimental data of recombinant Baby Hamster Kidney (BHK-21A) cultures producing a recombinant fusion glycoprotein. The identified EMs kinetics demonstrated typical glucose and glutamine metabolic responses during cell growth and IgG1-IL2 synthesis. Finally, an online optimisation study was conducted in which the optimal feeding strategies of glucose and glutamine were calculated after re-estimation of model parameters at each sampling time. An improvement in the final product concentration was obtained as a result of this online optimisation.

CONCLUSION

The main contribution of this work is a novel bioreactor optimal control method that uses detailed information concerning the metabolism of the underlying biological system. Moreover, the method allows the identification of structural modifications in metabolism over batch time.

摘要

背景

“组学”科学的进展使人们对许多具有工业价值的生物系统有了更深入的了解。然而,这些知识在生物反应器层面用于先进的生物过程监测和控制的情况仍然很少。在这项工作中,提出了一种基于所研究生物体代谢网络设计的生物过程控制方法。生物过程动力学采用混合严格/数据驱动系统来表述,其固有结构由代谢基本模式定义。

结果

将所研究系统的代谢网络分解为基本模式(EMs),这些基本模式是能够在稳态下连贯运行的最简单路径。得到了一种以连接底物与终产物的简化反应形式表示的简化反应机制。构建了一个整合物料平衡方程、基本模式反应化学计量学和动力学的动态混合系统。从过程优化的角度来看,基本模式动力学被定义为两项的乘积:一项是已知的机理/经验项,另一项是必须从数据中识别的未知项。这种方法能够量化各个基本模式所携带的通量,这对于识别作为环境条件函数的主导途径非常有帮助。该方法被用于分析生产重组融合糖蛋白的重组幼仓鼠肾(BHK - 21A)细胞培养的实验数据。所确定的基本模式动力学展示了细胞生长以及IgG1 - IL2合成过程中典型的葡萄糖和谷氨酰胺代谢响应。最后,进行了一项在线优化研究,在每个采样时间重新估计模型参数后计算葡萄糖和谷氨酰胺的最佳补料策略。通过这种在线优化,最终产物浓度得到了提高。

结论

这项工作的主要贡献是一种新颖的生物反应器最优控制方法,该方法使用了有关基础生物系统代谢的详细信息。此外,该方法还能够识别批次时间内代谢的结构变化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9b81/1800868/09cbbf0eb7eb/1471-2105-8-30-1.jpg

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