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谷氨酰胺供应控制的中国仓鼠卵巢细胞生长和代谢动力学。

Dynamics of growth and metabolism controlled by glutamine availability in Chinese hamster ovary cells.

机构信息

Biochemical Engineering Institute, Saarland University, Campus A1.5, 66123, Saarbrücken, Germany.

出版信息

Appl Microbiol Biotechnol. 2014 Feb;98(4):1771-83. doi: 10.1007/s00253-013-5452-2. Epub 2013 Dec 22.

Abstract

The physiology of animal cells is characterized by constantly changing environmental conditions and adapting cellular responses. Applied dynamic metabolic flux analysis captures metabolic dynamics and can be applied to industrially relevant cultivation conditions. We investigated the impact of glutamine availability or limitation on the physiology of CHO K1 cells in eight different batch and fed-batch cultivations. Varying glutamine availability resulted in global metabolic changes. We observed dose-dependent effects of glutamine in batch cultivation. Identifying metabolic links from the glutamine metabolism to specific metabolic pathways, we show that glutamine feeding results in its coupling to tricarboxylic acid cycle fluxes and in its decoupling from metabolic waste production. We provide a mechanistic explanation of the cellular responses upon mild or severe glutamine limitation and ammonia stress. The growth rate of CHO K1 decreased with increasing ammonia levels in the supernatant. On the other hand, growth, especially culture longevity, was stimulated at mild glutamine-limiting conditions. Flux rearrangements in the pyruvate and amino acid metabolism compensate glutamine limitation by consumption of alternative carbon sources and facilitating glutamine synthesis and mitigate ammonia stress as result of glutamine abundance.

摘要

动物细胞的生理学特点是不断变化的环境条件和适应性的细胞反应。应用动态代谢通量分析可以捕捉到代谢动力学,并可应用于工业相关的培养条件。我们研究了在八种不同的分批和补料分批培养中,谷氨酰胺的可用性或缺乏对 CHO K1 细胞生理学的影响。谷氨酰胺可用性的变化导致了全局代谢变化。我们在分批培养中观察到谷氨酰胺的剂量依赖性效应。从谷氨酰胺代谢到特定代谢途径的代谢联系,我们表明,谷氨酰胺喂养导致其与三羧酸循环通量偶联,并与其代谢废物产生解偶联。我们提供了在轻度或重度谷氨酰胺限制和氨应激下细胞反应的机制解释。上清液中氨水平的增加导致 CHO K1 的生长速率降低。另一方面,在轻度谷氨酰胺限制条件下,生长,特别是培养寿命,受到刺激。丙酮酸和氨基酸代谢中的通量重排通过消耗替代碳源来补偿谷氨酰胺限制,并促进谷氨酰胺合成,并减轻由于谷氨酰胺丰度导致的氨应激。

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