An accurate description of Aspergillus niger organic acid batch fermentation through dynamic metabolic modelling

Abstract Background Aspergillus niger fermentation has provided the chief source of industrial citric acid for over 50 years. Traditional strain development of this organism was achieved through random mutagenesis, but advances in genomics have enabled the development of genome-scale metabolic model...

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Main Authors: Daniel J. Upton, Simon J. McQueen-Mason, A. Jamie Wood
Format: Article
Language:English
Published: BMC 2017-11-01
Series:Biotechnology for Biofuels
Subjects:
Online Access:http://link.springer.com/article/10.1186/s13068-017-0950-6
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spelling doaj-93aa7693c23d4f58beb6af4a421d7e022020-11-25T00:30:29ZengBMCBiotechnology for Biofuels1754-68342017-11-0110111410.1186/s13068-017-0950-6An accurate description of Aspergillus niger organic acid batch fermentation through dynamic metabolic modellingDaniel J. Upton0Simon J. McQueen-Mason1A. Jamie Wood2Department of Biology, University of YorkDepartment of Biology, University of YorkDepartment of Biology, University of YorkAbstract Background Aspergillus niger fermentation has provided the chief source of industrial citric acid for over 50 years. Traditional strain development of this organism was achieved through random mutagenesis, but advances in genomics have enabled the development of genome-scale metabolic modelling that can be used to make predictive improvements in fermentation performance. The parent citric acid-producing strain of A. niger, ATCC 1015, has been described previously by a genome-scale metabolic model that encapsulates its response to ambient pH. Here, we report the development of a novel double optimisation modelling approach that generates time-dependent citric acid fermentation using dynamic flux balance analysis. Results The output from this model shows a good match with empirical fermentation data. Our studies suggest that citric acid production commences upon a switch to phosphate-limited growth and this is validated by fitting to empirical data, which confirms the diauxic growth behaviour and the role of phosphate storage as polyphosphate. Conclusions The calibrated time-course model reflects observed metabolic events and generates reliable in silico data for industrially relevant fermentative time series, and for the behaviour of engineered strains suggesting that our approach can be used as a powerful tool for predictive metabolic engineering.http://link.springer.com/article/10.1186/s13068-017-0950-6Aspergillus nigerCitric aciddFBAMetabolic modellingPolyphosphate
collection DOAJ
language English
format Article
sources DOAJ
author Daniel J. Upton
Simon J. McQueen-Mason
A. Jamie Wood
spellingShingle Daniel J. Upton
Simon J. McQueen-Mason
A. Jamie Wood
An accurate description of Aspergillus niger organic acid batch fermentation through dynamic metabolic modelling
Biotechnology for Biofuels
Aspergillus niger
Citric acid
dFBA
Metabolic modelling
Polyphosphate
author_facet Daniel J. Upton
Simon J. McQueen-Mason
A. Jamie Wood
author_sort Daniel J. Upton
title An accurate description of Aspergillus niger organic acid batch fermentation through dynamic metabolic modelling
title_short An accurate description of Aspergillus niger organic acid batch fermentation through dynamic metabolic modelling
title_full An accurate description of Aspergillus niger organic acid batch fermentation through dynamic metabolic modelling
title_fullStr An accurate description of Aspergillus niger organic acid batch fermentation through dynamic metabolic modelling
title_full_unstemmed An accurate description of Aspergillus niger organic acid batch fermentation through dynamic metabolic modelling
title_sort accurate description of aspergillus niger organic acid batch fermentation through dynamic metabolic modelling
publisher BMC
series Biotechnology for Biofuels
issn 1754-6834
publishDate 2017-11-01
description Abstract Background Aspergillus niger fermentation has provided the chief source of industrial citric acid for over 50 years. Traditional strain development of this organism was achieved through random mutagenesis, but advances in genomics have enabled the development of genome-scale metabolic modelling that can be used to make predictive improvements in fermentation performance. The parent citric acid-producing strain of A. niger, ATCC 1015, has been described previously by a genome-scale metabolic model that encapsulates its response to ambient pH. Here, we report the development of a novel double optimisation modelling approach that generates time-dependent citric acid fermentation using dynamic flux balance analysis. Results The output from this model shows a good match with empirical fermentation data. Our studies suggest that citric acid production commences upon a switch to phosphate-limited growth and this is validated by fitting to empirical data, which confirms the diauxic growth behaviour and the role of phosphate storage as polyphosphate. Conclusions The calibrated time-course model reflects observed metabolic events and generates reliable in silico data for industrially relevant fermentative time series, and for the behaviour of engineered strains suggesting that our approach can be used as a powerful tool for predictive metabolic engineering.
topic Aspergillus niger
Citric acid
dFBA
Metabolic modelling
Polyphosphate
url http://link.springer.com/article/10.1186/s13068-017-0950-6
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