A community-driven reconstruction of the Aspergillus niger metabolic network

Julian Brandl; Maria Victoria Aguilar-Pontes; Paul Schäpe; Anders Noerregaard; Mikko Arvas; Arthur F. J. Ram; Vera Meyer; Adrian Tsang; Ronald P. de Vries; Mikael R. Andersen

doi:10.1186/s40694-018-0060-7

Fungal Biology and Biotechnology (Sep 2018)

A community-driven reconstruction of the Aspergillus niger metabolic network

Julian Brandl,
Maria Victoria Aguilar-Pontes,
Paul Schäpe,
Anders Noerregaard,
Mikko Arvas,
Arthur F. J. Ram,
Vera Meyer,
Adrian Tsang,
Ronald P. de Vries,
Mikael R. Andersen

Affiliations

Julian Brandl: Technical University of Denmark
Maria Victoria Aguilar-Pontes: Fungal Physiology, Westerdijk Fungal Biodiversity Institute and Fungal Molecular Physiology, Utrecht University
Paul Schäpe: Berlin University of Technology
Anders Noerregaard: Technical University of Denmark
Mikko Arvas: VTT Technical Research Centre of Finland
Arthur F. J. Ram: Leiden University
Vera Meyer: Berlin University of Technology
Adrian Tsang: Concordia University
Ronald P. de Vries: Fungal Physiology, Westerdijk Fungal Biodiversity Institute and Fungal Molecular Physiology, Utrecht University
Mikael R. Andersen: Technical University of Denmark

DOI: https://doi.org/10.1186/s40694-018-0060-7
Journal volume & issue: Vol. 5, no. 1
pp. 1 – 12

Abstract

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Abstract Background Aspergillus niger is an important fungus used in industrial applications for enzyme and acid production. To enable rational metabolic engineering of the species, available information can be collected and integrated in a genome-scale model to devise strategies for improving its performance as a host organism. Results In this paper, we update an existing model of A. niger metabolism to include the information collected from 876 publications, thereby expanding the coverage of the model by 940 reactions, 777 metabolites and 454 genes. In the presented consensus genome-scale model of A. niger iJB1325 , we integrated experimental data from publications and patents, as well as our own experiments, into a consistent network. This information has been included in a standardized way, allowing for automated testing and continuous improvements in the future. This repository of experimental data allowed the definition of 471 individual test cases, of which the model complies with 373 of them. We further re-analyzed existing transcriptomics and quantitative physiology data to gain new insights on metabolism. Additionally, the model contains 3482 checks on the model structure, thereby representing the best validated genome-scale model on A. niger developed until now. Strain-specific model versions for strains ATCC 1015 and CBS 513.88 have been created containing all data used for model building, thereby allowing users to adopt the models and check the updated version against the experimental data. The resulting model is compliant with the SBML standard and therefore enables users to easily simulate it using their preferred software solution. Conclusion Experimental data on most organisms are scattered across hundreds of publications and several repositories.To allow for a systems level understanding of metabolism, the data must be integrated in a consistent knowledge network. The A. niger iJB1325 model presented here integrates the available data into a highly curated genome-scale model to facilitate the simulation of flux distributions, as well as the interpretation of other genome-scale data by providing the metabolic context.

Published in Fungal Biology and Biotechnology

ISSN: 2054-3085 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Technology: Chemical technology: Biotechnology
Website: https://fungalbiolbiotech.biomedcentral.com

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