Literature DB >> 29688451

Genome-scale metabolic modeling of responses to polymyxins in Pseudomonas aeruginosa.

Yan Zhu1, Tobias Czauderna2, Jinxin Zhao1, Matthias Klapperstueck2, Mohd Hafidz Mahamad Maifiah3, Mei-Ling Han3, Jing Lu4, Björn Sommer5, Tony Velkov6, Trevor Lithgow1, Jiangning Song1, Falk Schreiber2,5, Jian Li1.   

Abstract

Background: Pseudomonas aeruginosa often causes multidrug-resistant infections in immunocompromised patients, and polymyxins are often used as the last-line therapy. Alarmingly, resistance to polymyxins has been increasingly reported worldwide recently. To rescue this last-resort class of antibiotics, it is necessary to systematically understand how P. aeruginosa alters its metabolism in response to polymyxin treatment, thereby facilitating the development of effective therapies. To this end, a genome-scale metabolic model (GSMM) was used to analyze bacterial metabolic changes at the systems level. Findings: A high-quality GSMM iPAO1 was constructed for P. aeruginosa PAO1 for antimicrobial pharmacological research. Model iPAO1 encompasses an additional periplasmic compartment and contains 3022 metabolites, 4265 reactions, and 1458 genes in total. Growth prediction on 190 carbon and 95 nitrogen sources achieved an accuracy of 89.1%, outperforming all reported P. aeruginosa models. Notably, prediction of the essential genes for growth achieved a high accuracy of 87.9%. Metabolic simulation showed that lipid A modifications associated with polymyxin resistance exert a limited impact on bacterial growth and metabolism but remarkably change the physiochemical properties of the outer membrane. Modeling with transcriptomics constraints revealed a broad range of metabolic responses to polymyxin treatment, including reduced biomass synthesis, upregulated amino acid catabolism, induced flux through the tricarboxylic acid cycle, and increased redox turnover. Conclusions: Overall, iPAO1 represents the most comprehensive GSMM constructed to date for Pseudomonas. It provides a powerful systems pharmacology platform for the elucidation of complex killing mechanisms of antibiotics.

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Year:  2018        PMID: 29688451      PMCID: PMC6333913          DOI: 10.1093/gigascience/giy021

Source DB:  PubMed          Journal:  Gigascience        ISSN: 2047-217X            Impact factor:   6.524


  93 in total

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  18 in total

1.  Genome-scale metabolic modeling of responses to polymyxins in Pseudomonas aeruginosa.

Authors:  Yan Zhu; Tobias Czauderna; Jinxin Zhao; Matthias Klapperstueck; Mohd Hafidz Mahamad Maifiah; Mei-Ling Han; Jing Lu; Björn Sommer; Tony Velkov; Trevor Lithgow; Jiangning Song; Falk Schreiber; Jian Li
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