Multiplicity of steady states in glycolysis and shift of metabolic state in cultured mammalian cells.

Multiplicity of steady states in glycolysis and shift of metabolic state in cultured mammalian cells.

Cultured mammalian cells exhibit elevated glycolysis flux and high lactate production. In the industrial bioprocesses for biotherapeutic protein production, glucose is supplemented to the culture medium to sustain continued cell growth resulting in the accumulation of lactate to high levels. In such...

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Main Authors: Bhanu Chandra Mulukutla, Andrew Yongky, Simon Grimm, Prodromos Daoutidis, Wei-Shou Hu
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2015-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4373774?pdf=render
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spelling doaj-7b988fd8f51041bd8db15ce30ad127ff2020-11-24T21:24:18ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-01103e012156110.1371/journal.pone.0121561Multiplicity of steady states in glycolysis and shift of metabolic state in cultured mammalian cells.Bhanu Chandra MulukutlaAndrew YongkySimon GrimmProdromos DaoutidisWei-Shou HuCultured mammalian cells exhibit elevated glycolysis flux and high lactate production. In the industrial bioprocesses for biotherapeutic protein production, glucose is supplemented to the culture medium to sustain continued cell growth resulting in the accumulation of lactate to high levels. In such fed-batch cultures, sometimes a metabolic shift from a state of high glycolysis flux and high lactate production to a state of low glycolysis flux and low lactate production or even lactate consumption is observed. While in other cases with very similar culture conditions, the same cell line and medium, cells continue to produce lactate. A metabolic shift to lactate consumption has been correlated to the productivity of the process. Cultures that exhibited the metabolic shift to lactate consumption had higher titers than those which didn't. However, the cues that trigger the metabolic shift to lactate consumption state (or low lactate production state) are yet to be identified. Metabolic control of cells is tightly linked to growth control through signaling pathways such as the AKT pathway. We have previously shown that the glycolysis of proliferating cells can exhibit bistability with well-segregated high flux and low flux states. Low lactate production (or lactate consumption) is possible only at a low glycolysis flux state. In this study, we use mathematical modeling to demonstrate that lactate inhibition together with AKT regulation on glycolysis enzymes can profoundly influence the bistable behavior, resulting in a complex steady-state topology. The transition from the high flux state to the low flux state can only occur in certain regions of the steady state topology, and therefore the metabolic fate of the cells depends on their metabolic trajectory encountering the region that allows such a metabolic state switch. Insights from such switch behavior present us with new means to control the metabolism of mammalian cells in fed-batch cultures.http://europepmc.org/articles/PMC4373774?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Bhanu Chandra Mulukutla
Andrew Yongky
Simon Grimm
Prodromos Daoutidis
Wei-Shou Hu
spellingShingle Bhanu Chandra Mulukutla
Andrew Yongky
Simon Grimm
Prodromos Daoutidis
Wei-Shou Hu
Multiplicity of steady states in glycolysis and shift of metabolic state in cultured mammalian cells.
PLoS ONE
author_facet Bhanu Chandra Mulukutla
Andrew Yongky
Simon Grimm
Prodromos Daoutidis
Wei-Shou Hu
author_sort Bhanu Chandra Mulukutla
title Multiplicity of steady states in glycolysis and shift of metabolic state in cultured mammalian cells.
title_short Multiplicity of steady states in glycolysis and shift of metabolic state in cultured mammalian cells.
title_full Multiplicity of steady states in glycolysis and shift of metabolic state in cultured mammalian cells.
title_fullStr Multiplicity of steady states in glycolysis and shift of metabolic state in cultured mammalian cells.
title_full_unstemmed Multiplicity of steady states in glycolysis and shift of metabolic state in cultured mammalian cells.
title_sort multiplicity of steady states in glycolysis and shift of metabolic state in cultured mammalian cells.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2015-01-01
description Cultured mammalian cells exhibit elevated glycolysis flux and high lactate production. In the industrial bioprocesses for biotherapeutic protein production, glucose is supplemented to the culture medium to sustain continued cell growth resulting in the accumulation of lactate to high levels. In such fed-batch cultures, sometimes a metabolic shift from a state of high glycolysis flux and high lactate production to a state of low glycolysis flux and low lactate production or even lactate consumption is observed. While in other cases with very similar culture conditions, the same cell line and medium, cells continue to produce lactate. A metabolic shift to lactate consumption has been correlated to the productivity of the process. Cultures that exhibited the metabolic shift to lactate consumption had higher titers than those which didn't. However, the cues that trigger the metabolic shift to lactate consumption state (or low lactate production state) are yet to be identified. Metabolic control of cells is tightly linked to growth control through signaling pathways such as the AKT pathway. We have previously shown that the glycolysis of proliferating cells can exhibit bistability with well-segregated high flux and low flux states. Low lactate production (or lactate consumption) is possible only at a low glycolysis flux state. In this study, we use mathematical modeling to demonstrate that lactate inhibition together with AKT regulation on glycolysis enzymes can profoundly influence the bistable behavior, resulting in a complex steady-state topology. The transition from the high flux state to the low flux state can only occur in certain regions of the steady state topology, and therefore the metabolic fate of the cells depends on their metabolic trajectory encountering the region that allows such a metabolic state switch. Insights from such switch behavior present us with new means to control the metabolism of mammalian cells in fed-batch cultures.
url http://europepmc.org/articles/PMC4373774?pdf=render
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