Bedaquiline reprograms central metabolism to reveal glycolytic vulnerability in Mycobacterium tuberculosis

Jared S Mackenzie; Dirk A Lamprecht; Rukaya Asmal; John H Adamson; Khushboo Borah; Dany J V Beste; Bei Shi Lee; Kevin Pethe; Simon Rousseau; Inna Krieger; James C Sacchettini; Joel N Glasgow; Adrie J C Steyn

doi:10.1038/s41467-020-19959-4

Bedaquiline reprograms central metabolism to reveal glycolytic vulnerability in Mycobacterium tuberculosis

Nat Commun. 2020 Nov 30;11(1):6092. doi: 10.1038/s41467-020-19959-4.

Authors

Jared S Mackenzie¹, Dirk A Lamprecht², Rukaya Asmal¹, John H Adamson¹, Khushboo Borah³, Dany J V Beste³, Bei Shi Lee⁴, Kevin Pethe^{4

5}, Simon Rousseau⁶, Inna Krieger⁶, James C Sacchettini⁶, Joel N Glasgow⁷, Adrie J C Steyn^{8

9

10}

Affiliations

¹ Africa Health Research Institute, Durban, 4001, South Africa.
² Janssen Pharmaceutica, Global Public Health, Turnhoutseweg 30, 2340, Beerse, Belgium.
³ Faculty of Health and Medical Sciences, University of Surrey, Guildford, UK.
⁴ School of Biological Sciences, Nanyang Technological University, Singapore, Singapore.
⁵ Lee Kong Chian School of Medicine, Nanyang Technological University, Singapore, Singapore.
⁶ Texas A&M University, Department of Biochemistry and Biophysics, College Station, TX, USA.
⁷ Department of Microbiology, University of Alabama at Birmingham, Birmingham, AL, USA.
⁸ Africa Health Research Institute, Durban, 4001, South Africa. asteyn@uab.edu.
⁹ Department of Microbiology, University of Alabama at Birmingham, Birmingham, AL, USA. asteyn@uab.edu.
¹⁰ Center for AIDS Research and Center for Free Radical Biology, University of Alabama at Birmingham, Birmingham, AL, USA. asteyn@uab.edu.

Abstract

The approval of bedaquiline (BDQ) for the treatment of tuberculosis has generated substantial interest in inhibiting energy metabolism as a therapeutic paradigm. However, it is not known precisely how BDQ triggers cell death in Mycobacterium tuberculosis (Mtb). Using ¹³C isotopomer analysis, we show that BDQ-treated Mtb redirects central carbon metabolism to induce a metabolically vulnerable state susceptible to genetic disruption of glycolysis and gluconeogenesis. Metabolic flux profiles indicate that BDQ-treated Mtb is dependent on glycolysis for ATP production, operates a bifurcated TCA cycle by increasing flux through the glyoxylate shunt, and requires enzymes of the anaplerotic node and methylcitrate cycle. Targeting oxidative phosphorylation (OXPHOS) with BDQ and simultaneously inhibiting substrate level phosphorylation via genetic disruption of glycolysis leads to rapid sterilization. Our findings provide insight into the metabolic mechanism of BDQ-induced cell death and establish a paradigm for the development of combination therapies that target OXPHOS and glycolysis.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Anti-Bacterial Agents / pharmacology*
Antitubercular Agents / pharmacology
Bacterial Proteins / metabolism
Carbon Cycle / drug effects
Citric Acid Cycle / drug effects
Diarylquinolines / pharmacology*
Energy Metabolism / drug effects
Glycolysis / drug effects*
Glyoxylates
Mycobacterium tuberculosis / drug effects*
Mycobacterium tuberculosis / genetics
Mycobacterium tuberculosis / metabolism*
Oxidative Phosphorylation
Tuberculosis / microbiology

Substances

Anti-Bacterial Agents
Antitubercular Agents
Bacterial Proteins
Diarylquinolines
Glyoxylates
bedaquiline
glyoxylic acid

Abstract

Publication types

MeSH terms

Substances

Grants and funding