Degeneration of penicillin production in ethanol-limited chemostat cultivations of Penicillium chrysogenum: A systems biology approach

BACKGROUND: In microbial production of non-catabolic products such as antibiotics a loss of production capacity upon long-term cultivation (for example chemostat), a phenomenon called strain degeneration, is often observed. In this study a systems biology approach, monitoring changes from gene to pr...

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Autores principales: Douma, Rutger D, Batista, Joana M, Touw, Kai M, Kiel, Jan AKW, Krikken, Arjen M, Zhao, Zheng, Veiga, Tânia, Klaassen, Paul, Bovenberg, Roel AL, Daran, Jean-Marc, Heijnen, Joseph J, van Gulik, Walter M
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2011
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3224390/
https://www.ncbi.nlm.nih.gov/pubmed/21854586
http://dx.doi.org/10.1186/1752-0509-5-132
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author Douma, Rutger D
Batista, Joana M
Touw, Kai M
Kiel, Jan AKW
Krikken, Arjen M
Zhao, Zheng
Veiga, Tânia
Klaassen, Paul
Bovenberg, Roel AL
Daran, Jean-Marc
Heijnen, Joseph J
van Gulik, Walter M
author_facet Douma, Rutger D
Batista, Joana M
Touw, Kai M
Kiel, Jan AKW
Krikken, Arjen M
Zhao, Zheng
Veiga, Tânia
Klaassen, Paul
Bovenberg, Roel AL
Daran, Jean-Marc
Heijnen, Joseph J
van Gulik, Walter M
author_sort Douma, Rutger D
collection PubMed
description BACKGROUND: In microbial production of non-catabolic products such as antibiotics a loss of production capacity upon long-term cultivation (for example chemostat), a phenomenon called strain degeneration, is often observed. In this study a systems biology approach, monitoring changes from gene to produced flux, was used to study degeneration of penicillin production in a high producing Penicillium chrysogenum strain during prolonged ethanol-limited chemostat cultivations. RESULTS: During these cultivations, the biomass specific penicillin production rate decreased more than 10-fold in less than 22 generations. No evidence was obtained for a decrease of the copy number of the penicillin gene cluster, nor a significant down regulation of the expression of the penicillin biosynthesis genes. However, a strong down regulation of the biosynthesis pathway of cysteine, one of the precursors of penicillin, was observed. Furthermore the protein levels of the penicillin pathway enzymes L-α-(δ-aminoadipyl)-L-α-cystenyl-D-α-valine synthetase (ACVS) and isopenicillin-N synthase (IPNS), decreased significantly. Re-cultivation of fully degenerated cells in unlimited batch culture and subsequent C-limited chemostats did only result in a slight recovery of penicillin production. CONCLUSIONS: Our findings indicate that the observed degeneration is attributed to a significant decrease of the levels of the first two enzymes of the penicillin biosynthesis pathway, ACVS and IPNS. This decrease is not caused by genetic instability of the penicillin amplicon, neither by down regulation of the penicillin biosynthesis pathway. Furthermore no indications were obtained for degradation of these enzymes as a result of autophagy. Possible causes for the decreased enzyme levels could be a decrease of the translation efficiency of ACVS and IPNS during degeneration, or the presence of a culture variant impaired in the biosynthesis of functional proteins of these enzymes, which outcompeted the high producing part of the population.
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spelling pubmed-32243902011-11-30 Degeneration of penicillin production in ethanol-limited chemostat cultivations of Penicillium chrysogenum: A systems biology approach Douma, Rutger D Batista, Joana M Touw, Kai M Kiel, Jan AKW Krikken, Arjen M Zhao, Zheng Veiga, Tânia Klaassen, Paul Bovenberg, Roel AL Daran, Jean-Marc Heijnen, Joseph J van Gulik, Walter M BMC Syst Biol Research Article BACKGROUND: In microbial production of non-catabolic products such as antibiotics a loss of production capacity upon long-term cultivation (for example chemostat), a phenomenon called strain degeneration, is often observed. In this study a systems biology approach, monitoring changes from gene to produced flux, was used to study degeneration of penicillin production in a high producing Penicillium chrysogenum strain during prolonged ethanol-limited chemostat cultivations. RESULTS: During these cultivations, the biomass specific penicillin production rate decreased more than 10-fold in less than 22 generations. No evidence was obtained for a decrease of the copy number of the penicillin gene cluster, nor a significant down regulation of the expression of the penicillin biosynthesis genes. However, a strong down regulation of the biosynthesis pathway of cysteine, one of the precursors of penicillin, was observed. Furthermore the protein levels of the penicillin pathway enzymes L-α-(δ-aminoadipyl)-L-α-cystenyl-D-α-valine synthetase (ACVS) and isopenicillin-N synthase (IPNS), decreased significantly. Re-cultivation of fully degenerated cells in unlimited batch culture and subsequent C-limited chemostats did only result in a slight recovery of penicillin production. CONCLUSIONS: Our findings indicate that the observed degeneration is attributed to a significant decrease of the levels of the first two enzymes of the penicillin biosynthesis pathway, ACVS and IPNS. This decrease is not caused by genetic instability of the penicillin amplicon, neither by down regulation of the penicillin biosynthesis pathway. Furthermore no indications were obtained for degradation of these enzymes as a result of autophagy. Possible causes for the decreased enzyme levels could be a decrease of the translation efficiency of ACVS and IPNS during degeneration, or the presence of a culture variant impaired in the biosynthesis of functional proteins of these enzymes, which outcompeted the high producing part of the population. BioMed Central 2011-08-19 /pmc/articles/PMC3224390/ /pubmed/21854586 http://dx.doi.org/10.1186/1752-0509-5-132 Text en Copyright ©2011 Douma et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Douma, Rutger D
Batista, Joana M
Touw, Kai M
Kiel, Jan AKW
Krikken, Arjen M
Zhao, Zheng
Veiga, Tânia
Klaassen, Paul
Bovenberg, Roel AL
Daran, Jean-Marc
Heijnen, Joseph J
van Gulik, Walter M
Degeneration of penicillin production in ethanol-limited chemostat cultivations of Penicillium chrysogenum: A systems biology approach
title Degeneration of penicillin production in ethanol-limited chemostat cultivations of Penicillium chrysogenum: A systems biology approach
title_full Degeneration of penicillin production in ethanol-limited chemostat cultivations of Penicillium chrysogenum: A systems biology approach
title_fullStr Degeneration of penicillin production in ethanol-limited chemostat cultivations of Penicillium chrysogenum: A systems biology approach
title_full_unstemmed Degeneration of penicillin production in ethanol-limited chemostat cultivations of Penicillium chrysogenum: A systems biology approach
title_short Degeneration of penicillin production in ethanol-limited chemostat cultivations of Penicillium chrysogenum: A systems biology approach
title_sort degeneration of penicillin production in ethanol-limited chemostat cultivations of penicillium chrysogenum: a systems biology approach
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3224390/
https://www.ncbi.nlm.nih.gov/pubmed/21854586
http://dx.doi.org/10.1186/1752-0509-5-132
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