Catalase activity deficiency sensitizes multidrug-resistant Mycobacterium tuberculosis to the ATP synthase inhibitor bedaquiline.

Publication date: Nov 13, 2024

Multidrug-resistant tuberculosis (MDR-TB), defined as resistance to the first-line drugs isoniazid and rifampin, is a growing source of global mortality and threatens global control of tuberculosis disease. The diarylquinoline bedaquiline has recently emerged as a highly efficacious drug against MDR-TB and kills Mycobacterium tuberculosis by inhibiting mycobacterial ATP synthase. However, the mechanisms underlying bedaquiline’s efficacy against MDR-TB remain unknown. Here we investigate bedaquiline hyper-susceptibility in drug-resistant Mycobacterium tuberculosis using systems biology approaches. We discovered that MDR clinical isolates are commonly sensitized to bedaquiline. This hypersensitization is caused by several physiological changes induced by deficient catalase activity. These include enhanced accumulation of reactive oxygen species, increased susceptibility to DNA damage, induction of sensitizing transcriptional programs, and metabolic repression of several biosynthetic pathways. In this work we demonstrate how resistance-associated changes in bacterial physiology can mechanistically induce collateral antimicrobial drug sensitivity and reveal druggable vulnerabilities in antimicrobial resistant pathogens.

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Concepts Keywords
Atp Antitubercular Agents
Diarylquinoline Antitubercular Agents
Mechanisticallyinduce Bacterial Proteins
Mycobacterialatp Bacterial Proteins
Tuberculosis bedaquiline
Catalase
Catalase
Diarylquinolines
Diarylquinolines
DNA Damage
Humans
Microbial Sensitivity Tests
Mycobacterium tuberculosis
Reactive Oxygen Species
Reactive Oxygen Species
Tuberculosis, Multidrug-Resistant

Semantics

Type Source Name
drug DRUGBANK ATP
drug DRUGBANK Bedaquiline
disease MESH Multidrug-resistant tuberculosis
drug DRUGBANK Isoniazid
drug DRUGBANK Rifampicin
disease MESH tuberculosis
pathway KEGG Tuberculosis
disease IDO susceptibility
disease MESH DNA damage
disease MESH repression
drug DRUGBANK Pretomanid
drug DRUGBANK Linezolid
drug DRUGBANK Moxifloxacin
drug DRUGBANK Nadide
disease IDO bactericidal
drug DRUGBANK Oxygen
pathway KEGG Folate biosynthesis
drug DRUGBANK Coenzyme M
drug DRUGBANK Methyl isocyanate
drug DRUGBANK Timonacic
disease IDO bacteria
disease MESH oxidative stress
drug DRUGBANK Trestolone
drug DRUGBANK Proline
pathway KEGG Carbon metabolism
drug DRUGBANK Nigericin
disease MESH catalase deficiency
disease IDO production
pathway KEGG Cholesterol metabolism
pathway REACTOME Base Excision Repair
pathway KEGG Homologous recombination
pathway REACTOME Metabolism
drug DRUGBANK Esomeprazole
drug DRUGBANK Isoxaflutole
disease IDO process
drug DRUGBANK Tetrahydrofolic acid
pathway REACTOME Nucleotide biosynthesis
pathway KEGG Nucleotide metabolism
disease IDO replication
drug DRUGBANK Folic Acid
drug DRUGBANK Trimethoprim
drug DRUGBANK Thymidine monophosphate
drug DRUGBANK Sulfamethoxazole
disease MESH defects
drug DRUGBANK Phosphate ion
pathway KEGG Metabolic pathways
drug DRUGBANK L-Phenylalanine
drug DRUGBANK Coenzyme A
disease IDO drug susceptibility
disease MESH reinfection
disease MESH hypersensitivity
disease IDO bacteriostatic
drug DRUGBANK Aminosalicylic Acid
drug DRUGBANK N-Cyclohexyltaurine
disease MESH clinical relevance
pathway KEGG Oxidative phosphorylation
drug DRUGBANK Tetracycline
drug DRUGBANK Oleic Acid
drug DRUGBANK Dextrose unspecified form
drug DRUGBANK Tyloxapol
drug DRUGBANK Glycerin
drug DRUGBANK Pantothenic acid
drug DRUGBANK L-Leucine
drug DRUGBANK Methionine
disease IDO colony
drug DRUGBANK Naproxen
disease IDO cell
disease IDO reagent
drug DRUGBANK Lysozyme
disease IDO assay
drug DRUGBANK Zoledronic acid
drug DRUGBANK Water
drug DRUGBANK Trifluoro-thiamin phosphate
drug DRUGBANK Rifapentine
disease MESH extensively drug resistant tuberculosis
drug DRUGBANK NADH
disease MESH Hards
disease IDO antibiotic resistance
disease MESH hypoxia
drug DRUGBANK Guanine
disease MESH death
drug DRUGBANK Cyanocobalamin
pathway REACTOME Fatty acids
disease MESH relapse
disease MESH pulmonary tuberculosis
drug DRUGBANK Clofazimine
drug DRUGBANK Activated charcoal
drug DRUGBANK Nitrogen
disease MESH Infection
drug DRUGBANK (S)-Des-Me-Ampa
drug DRUGBANK Amber
pathway REACTOME Reproduction

Original Article

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