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通过基因组规模建模阐明分批补料培养中杂交瘤细胞的代谢。

Elucidation of metabolism in hybridoma cells grown in fed-batch culture by genome-scale modeling.

作者信息

Selvarasu Suresh, Wong Victor V T, Karimi Iftekhar A, Lee Dong-Yup

机构信息

Department of Chemical and Biomolecular Engineering, National University of Singapore, 4 Engineering Drive 4, Singapore 117576, Singapore.

出版信息

Biotechnol Bioeng. 2009 Apr 1;102(5):1494-504. doi: 10.1002/bit.22186.

DOI:10.1002/bit.22186
PMID:19048615
Abstract

Genome-scale modeling of mouse hybridoma cells producing monoclonal antibodies (mAb) was performed to elucidate their physiological and metabolic states during fed-batch cell culture. Initially, feed media nutrients were monitored to identify key components among carbon sources and amino acids with significant impact on the desired outcome, for example, cell growth and antibody production. The monitored profiles indicated rapid assimilation of glucose and glutamine during the exponential growth phase. Significant increase in mAb concentration was also observed when glutamine concentration was controlled at 0.5 mM as a feeding strategy. Based on the reconstructed genome-scale metabolic network of mouse hybridoma cells and fed-batch profiles, flux analysis was then implemented to investigate the cellular behavior and changes in internal fluxes during the cell culture. The simulated profile of the cell growth was consistent with experimentally measured specific growth rate. The in silico simulation results indicated (i) predominant utilization of glycolytic pathway for ATP production, (ii) importance of pyruvate node in metabolic shifting, and (iii) characteristic pattern in lactate to glucose ratio during the exponential phase. In future, experimental and in silico analyses can serve as a promising approach to identifying optimal feeding strategies and potential cell engineering targets as well as facilitate media optimization for the enhanced production of mAb or recombinant proteins in mammalian cells.

摘要

为阐明小鼠杂交瘤细胞在补料分批培养过程中的生理和代谢状态,对产生单克隆抗体(mAb)的小鼠杂交瘤细胞进行了全基因组规模建模。最初,监测补料培养基中的营养成分,以确定碳源和氨基酸中对预期结果(如细胞生长和抗体产生)有重大影响的关键成分。监测结果表明,在指数生长期葡萄糖和谷氨酰胺被快速同化。当将谷氨酰胺浓度控制在0.5 mM作为补料策略时,还观察到单克隆抗体浓度显著增加。基于重建的小鼠杂交瘤细胞全基因组规模代谢网络和补料分批培养曲线,随后进行通量分析,以研究细胞培养过程中的细胞行为和内部通量变化。模拟的细胞生长曲线与实验测量的比生长速率一致。计算机模拟结果表明:(i)糖酵解途径在ATP产生中占主导地位;(ii)丙酮酸节点在代谢转换中的重要性;(iii)指数期乳酸与葡萄糖比率的特征模式。未来,实验分析和计算机模拟分析可作为一种有前景的方法,用于确定最佳补料策略和潜在的细胞工程靶点,以及促进培养基优化,以提高哺乳动物细胞中单克隆抗体或重组蛋白的产量。

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