Bismuth-based drugs sensitize Pseudomonas aeruginosa to multiple antibiotics by disrupting iron homeostasis.
Yushan XiaXueying WeiPeng GaoChenyuan WangAnne de JongJonathan Hon Kwan ChenMaría José Rodríguez-SánchezAlba Rodríguez-NogalesPatricia Diez-EchaveJulio GálvezFederico GarciaWeihui WuRichard Yi-Tsun KaoHongyan LiRubén CebriánOscar Paul KuipersHongzhe SunPublished in: Nature microbiology (2024)
Pseudomonas aeruginosa infections are difficult to treat due to rapid development of antibiotic drug resistance. The synergistic combination of already-in-use drugs is an alternative to developing new antibiotics to combat antibiotic-resistant bacteria. Here we demonstrate that bismuth-based drugs (bismuth subsalicylate, colloidal bismuth subcitrate) in combination with different classes of antibiotics (tetracyclines, macrolides, quinolones, rifamycins and so on) can eliminate multidrug-resistant P. aeruginosa and do not induce development of antibiotic resistance. Bismuth disrupts iron homeostasis by binding to P. aeruginosa siderophores. Inside cells, bismuth inhibits the electron transport chain, dissipates the proton motive force and impairs efflux pump activity by disrupting iron-sulfur cluster-containing enzymes, including respiration complexes. As a result, bismuth facilitates antibiotic accumulation inside bacteria, enhancing their efficacy. The combination therapy shows potent antibacterial efficacy and low toxicity in an ex vivo bacteraemia model and increases the survival rate of mice in in vivo mouse lung-infection models. Our findings highlight the potential of bismuth-based drugs to be repurposed to combat P. aeruginosa infections in combination with clinically used antibiotics.
Keyphrases
- oxide nanoparticles
- pseudomonas aeruginosa
- visible light
- multidrug resistant
- combination therapy
- acinetobacter baumannii
- induced apoptosis
- oxidative stress
- staphylococcus aureus
- drug resistant
- type diabetes
- biofilm formation
- signaling pathway
- free survival
- gram negative
- single molecule
- drug delivery
- drug induced
- cancer therapy
- candida albicans
- wild type
- wound healing