AI Article Synopsis

  • Polymicrobial infections, especially involving Candida albicans and Pseudomonas aeruginosa, are difficult to treat due to limited understanding of pathogen interactions and drug effectiveness.
  • The study examined the effects of antifungal fluconazole (FLC) during co-infection using a zebrafish model, finding that P. aeruginosa actually enhances the efficacy of FLC against C. albicans.
  • This enhancement in treatment is partly attributed to "iron piracy," where the bacterial pathogen competes for iron, highlighting the importance of studying drug interactions in complex microbial environments.

Article Abstract

Polymicrobial infections are challenging to treat because we don't fully understand how pathogens interact during infection and how these interactions affect drug efficacy. Candida albicans and Pseudomonas aeruginosa are opportunistic pathogens that can be found in similar sites of infection such as in burn wounds and most importantly in the lungs of CF and mechanically ventilated patients. C. albicans is particularly difficult to treat because of the paucity of antifungal agents, some of which lack fungicidal activity. In this study, we investigated the efficacy of anti-fungal treatment during C. albicans-P. aeruginosa coculture and co-infection in the mucosal zebrafish infection model analogous to the lung. We find that P. aeruginosa enhances the activity of fluconazole (FLC), an anti-fungal drug that is fungistatic , to promote both clearance of C. albicans during co-infection and fungal killing . This synergy between FLC treatment and bacterial antagonism is partly due to iron piracy, as it is reduced upon iron supplementation and knockout of bacterial siderophores. Our work demonstrates that FLC has enhanced activity in clinically relevant contexts and highlights the need to understand antimicrobial effectiveness in the complex environment of the host with its associated microbial communities.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9022521PMC
http://dx.doi.org/10.1128/iai.00626-21DOI Listing

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