The antibiotic bedaquiline activates host macrophage innate immune resistance to bacterial infection.
Alexandre Giraud-GatineauJuan Manuel CoyaAlexandra MaureAnne BitonMichael ThomsonElliott M BernardJade MarrecMaximiliano G GutierrezGérald Larrouy-MaumusRoland BroschBrigitte GicquelLudovic TailleuxPublished in: eLife (2020)
Antibiotics are widely used in the treatment of bacterial infections. Although known for their microbicidal activity, antibiotics may also interfere with the host's immune system. Here, we analyzed the effects of bedaquiline (BDQ), an inhibitor of the mycobacterial ATP synthase, on human macrophages. Genome-wide gene expression analysis revealed that BDQ reprogramed cells into potent bactericidal phagocytes. We found that 579 and 1,495 genes were respectively differentially expressed in naive- and M. tuberculosis-infected macrophages incubated with the drug, with an over-representation of lysosome-associated genes. BDQ treatment triggered a variety of antimicrobial defense mechanisms, including phagosome-lysosome fusion, and autophagy. These effects were associated with activation of transcription factor EB, involved in the transcription of lysosomal genes, resulting in enhanced intracellular killing of different bacterial species that were naturally insensitive to BDQ. Thus, BDQ could be used as a host-directed therapy against a wide range of bacterial infections.
Keyphrases
- genome wide
- genome wide identification
- transcription factor
- innate immune
- dna methylation
- drug resistant
- mycobacterium tuberculosis
- multidrug resistant
- copy number
- endothelial cells
- bioinformatics analysis
- oxidative stress
- living cells
- stem cells
- adipose tissue
- gene expression
- staphylococcus aureus
- cell proliferation
- hepatitis c virus
- hiv aids
- anti inflammatory
- dna binding
- human immunodeficiency virus