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哺乳动物细胞连续培养中具有不同细胞代谢的多个稳态

Multiple steady states with distinct cellular metabolism in continuous culture of mammalian cells.

作者信息

Europa A F, Gambhir A, Fu P C, Hu W S

机构信息

Department of Chemical Engineering and Materials Science, 421 Washington Avenue SE, University of Minnesota, Minneapolis, MN 55455-0132, USA.

出版信息

Biotechnol Bioeng. 2000 Jan 5;67(1):25-34. doi: 10.1002/(sici)1097-0290(20000105)67:1<25::aid-bit4>3.0.co;2-k.

Abstract

Mammalian cells have the ability to proliferate under different nutrient environments by utilizing different combinations of the nutrients, especially glucose and the amino acids. Under the conditions often used in in vitro cultivation, the cells consume glucose and amino acids in great excess of what is needed for making up biomass and products. They also produce large amounts of metabolites with lactate, ammonia, and some non-essential amino acids such as alanine as the most dominant ones. By controlling glucose and glutamine at low levels, cellular metabolism can be altered and can result in reduced glucose and glutamine consumption as well as in reduced metabolite formation. Using a fed-batch reactor to manipulate glucose at a low level (as compared to a typical batch culture), cell metabolism was altered to a state with substantially reduced lactate production. The culture was then switched to a continuous mode and allowed to reach a steady-state. At this steady-state, the concentrations of cells and antibody were substantially higher than a control culture that was initiated from a batch culture without first altering cellular metabolism. The lactate and other metabolite concentrations were also substantially reduced as compared to the control culture. This newly observed steady-state was achieved at the same dilution rate and feed medium as the control culture. The paths leading to the two steady-states, however, were different. These results demonstrate steady-state multiplicity. At this new steady-state, not only was glucose metabolism altered, but the metabolism of amino acids was altered as well. The amino acid metabolism in the new steady-state was more balanced, and the excretion of non-essential amino acids and ammonia was substantially lower. This approach of reaching a more desirable steady-state with higher concentrations of cells and product opens a new avenue for high-density- and high-productivity-cell culture.

摘要

哺乳动物细胞能够通过利用不同的营养组合,特别是葡萄糖和氨基酸,在不同的营养环境下增殖。在体外培养常用的条件下,细胞消耗的葡萄糖和氨基酸大大超过了用于合成生物量和产物所需的量。它们还会产生大量代谢产物,其中乳酸、氨以及一些非必需氨基酸(如丙氨酸)最为主要。通过将葡萄糖和谷氨酰胺控制在低水平,可以改变细胞代谢,从而减少葡萄糖和谷氨酰胺的消耗以及代谢产物的形成。使用补料分批反应器将葡萄糖控制在低水平(与典型的分批培养相比),细胞代谢被改变为乳酸产量大幅降低的状态。然后将培养切换到连续模式并使其达到稳态。在这个稳态下,细胞和抗体的浓度显著高于从没有先改变细胞代谢的分批培养开始的对照培养。与对照培养相比,乳酸和其他代谢产物的浓度也显著降低。这个新观察到的稳态是在与对照培养相同的稀释率和进料培养基下实现的。然而,通向这两个稳态的途径不同。这些结果证明了稳态多重性。在这个新的稳态下,不仅葡萄糖代谢发生了改变,氨基酸代谢也发生了改变。新稳态下的氨基酸代谢更加平衡,非必需氨基酸和氨的排泄显著降低。这种达到具有更高细胞和产物浓度的更理想稳态的方法为高密度和高生产率细胞培养开辟了一条新途径。

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