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在晚期非生长阶段对 CHO 细胞代谢的代谢通量分析。

Metabolic flux analysis of CHO cell metabolism in the late non-growth phase.

机构信息

School of Chemical Engineering, Purdue University, West Lafayette, Indiana 47907, USA.

出版信息

Biotechnol Bioeng. 2011 Jan;108(1):82-92. doi: 10.1002/bit.22890.

Abstract

Chinese hamster ovary (CHO) cell cultures are commonly used for production of recombinant human therapeutic proteins. Often the goal of such a process is to separate the growth phase of the cells, from the non-growth phase where ideally the cells are diverting resources to produce the protein of interest. Characterizing the way that the cells use nutrients in terms of metabolic fluxes as a function of culture conditions can provide a deeper understanding of the cell biology offering guidance for process improvements. To evaluate the fluxes, metabolic flux analysis of the CHO cell culture in the non-growth phase was performed by a combination of steady-state isotopomer balancing and stoichiometric modeling. Analysis of the glycolytic pathway and pentose phosphate pathway (PPP) indicated that almost all of the consumed glucose is diverted towards PPP with a high NADPH production; with even recycle from PPP to G6P in some cases. Almost all of the pyruvate produced from glycolysis entered the TCA cycle with little or no lactate production. Comparison of the non-growth phase against previously reported fluxes from growth phase cultures indicated marked differences in the fluxes, in terms of the split between glycolysis and PPP, and also around the pyruvate node. Possible reasons for the high NADPH production are also discussed. Evaluation of the fluxes indicated that the medium strength, carbon dioxide level, and temperature with dissolved oxygen have statistically significant impacts on different nodes of the flux network.

摘要

中国仓鼠卵巢(CHO)细胞培养物通常用于生产重组人治疗蛋白。通常,此类过程的目标是将细胞的生长阶段与非生长阶段分开,在非生长阶段,细胞理想地将资源转移到生产感兴趣的蛋白质上。根据培养条件,以代谢通量的形式描述细胞利用营养物质的方式,可以更深入地了解细胞生物学,为工艺改进提供指导。为了评估通量,通过稳态同位素平衡和计量建模的组合,对非生长阶段 CHO 细胞培养物的代谢通量进行了分析。对糖酵解途径和戊糖磷酸途径(PPP)的分析表明,几乎所有消耗的葡萄糖都被转移到 PPP 中,产生大量的 NADPH;在某些情况下,甚至从 PPP 循环到 G6P。几乎所有来自糖酵解的丙酮酸都进入 TCA 循环,几乎没有或没有乳酸生成。将非生长阶段与先前报道的生长阶段培养物的通量进行比较表明,在糖酵解和 PPP 之间的分配以及丙酮酸节点周围,通量存在明显差异。还讨论了 NADPH 产量高的可能原因。通量评估表明,培养基强度、二氧化碳水平、溶解氧的温度对通量网络的不同节点有统计学显著影响。

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