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GSMN-ML- a genome scale metabolic network reconstruction of the obligate human pathogen Mycobacterium leprae

Khushboo Borah, Jacque-Lucca Kearney, Ruma Banerjee, View ORCID ProfilePankaj Vats, Huihai Wu, Sonal Dahale, Manjari K Sunitha, Rajendra Joshi, View ORCID ProfileBhushan Bonde, View ORCID ProfileOlabisi Ojo, Ramanuj Lahiri, Diana L. Williams, View ORCID ProfileJohnjoe McFadden
doi: https://doi.org/10.1101/819508
Khushboo Borah
1Faculty of Health and Medical Sciences, University of Surrey, Guildford, GU2 7XH, UK
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Jacque-Lucca Kearney
2Robens Centre for Public and Environmental Health, University of Surrey, GU27XH, UK
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Ruma Banerjee
3HPC-Medical and Bioinformatics Applications Group, Centre for Development of Advanced Computing, Pune University Campus, Pune-411007, INDIA
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Pankaj Vats
3HPC-Medical and Bioinformatics Applications Group, Centre for Development of Advanced Computing, Pune University Campus, Pune-411007, INDIA
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Huihai Wu
1Faculty of Health and Medical Sciences, University of Surrey, Guildford, GU2 7XH, UK
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Sonal Dahale
3HPC-Medical and Bioinformatics Applications Group, Centre for Development of Advanced Computing, Pune University Campus, Pune-411007, INDIA
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Manjari K Sunitha
3HPC-Medical and Bioinformatics Applications Group, Centre for Development of Advanced Computing, Pune University Campus, Pune-411007, INDIA
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Rajendra Joshi
3HPC-Medical and Bioinformatics Applications Group, Centre for Development of Advanced Computing, Pune University Campus, Pune-411007, INDIA
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Bhushan Bonde
4Head of Innovation Development, IT-Early Solutions, UCB Pharma, Slough, SL1 3WE
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Olabisi Ojo
5Department of Biological Sciences, Albany state university, GA 31705, USA
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Ramanuj Lahiri
6National Hansen’s Disease Program, Health Resources and Services Administration, Baton Rouge, LA 70803, USA
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Diana L. Williams
6National Hansen’s Disease Program, Health Resources and Services Administration, Baton Rouge, LA 70803, USA
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Johnjoe McFadden
1Faculty of Health and Medical Sciences, University of Surrey, Guildford, GU2 7XH, UK
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  • For correspondence: j.mcfadden@surrey.ac.uk
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Abstract

Leprosy, caused by Mycobacterium leprae, has plagued humanity for thousands of years and continues to cause morbidity, disability and stigmatization in two to three million people today. Although effective treatment is available, the disease incidence has remained approximately constant for decades so new approaches, such as vaccine or new drugs, are urgently needed for control. Research is however hampered by the pathogen’s obligate intracellular lifestyle and the fact that it has never been grown in vitro. Consequently, despite the availability of its complete genome sequence, fundamental questions regarding the biology of the pathogen, such as its metabolism, remain largely unexplored. In order to explore the metabolism of the leprosy bacillus with a long-term aim of developing a medium to grow the pathogen in vitro, we reconstructed an in silico genome scale metabolic model of the bacillus, GSMN-ML. The model was used to explore the growth and biomass production capabilities of the pathogen with a range of nutrient sources, such as amino acids, glucose, glycerol and metabolic intermediates. We also used the model to analyze RNA-seq data from M. leprae grown in mouse foot pads, and performed Differential Producibility Analysis (DPA) to identify metabolic pathways that appear to be active during intracellular growth of the pathogen, which included pathways for central carbon metabolism, co-factor, lipids, amino acids, nucleotides and cell wall synthesis. The GSMN-ML model is thereby a useful in silico tool that can be used to explore the metabolism of the leprosy bacillus, analyze functional genomic experimental data, generate predictions of nutrients required for growth of the bacillus in vitro and identify novel drug targets.

Author Summary Mycobacterium leprae, the obligate human pathogen is uncultivable in axenic growth medium, and this hinders research on this pathogen, and the pathogenesis of leprosy. The development of novel therapeutics relies on the understanding of growth, survival and metabolism of this bacterium in the host, the knowledge of which is currently very limited. Here we reconstructed a metabolic network of M. leprae-GSMN-ML, a powerful in silico tool to study growth and metabolism of the leprosy bacillus. We demonstrate the application of GSMN-ML to identify the metabolic pathways, and metabolite classes that M. leprae utilizes during intracellular growth.

Copyright 
The copyright holder for this preprint is the author/funder, who has granted bioRxiv a license to display the preprint in perpetuity. This article is a US Government work. It is not subject to copyright under 17 USC 105 and is also made available for use under a CC0 license.
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Posted October 25, 2019.
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GSMN-ML- a genome scale metabolic network reconstruction of the obligate human pathogen Mycobacterium leprae
Khushboo Borah, Jacque-Lucca Kearney, Ruma Banerjee, Pankaj Vats, Huihai Wu, Sonal Dahale, Manjari K Sunitha, Rajendra Joshi, Bhushan Bonde, Olabisi Ojo, Ramanuj Lahiri, Diana L. Williams, Johnjoe McFadden
bioRxiv 819508; doi: https://doi.org/10.1101/819508
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GSMN-ML- a genome scale metabolic network reconstruction of the obligate human pathogen Mycobacterium leprae
Khushboo Borah, Jacque-Lucca Kearney, Ruma Banerjee, Pankaj Vats, Huihai Wu, Sonal Dahale, Manjari K Sunitha, Rajendra Joshi, Bhushan Bonde, Olabisi Ojo, Ramanuj Lahiri, Diana L. Williams, Johnjoe McFadden
bioRxiv 819508; doi: https://doi.org/10.1101/819508

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