AI Article Synopsis

  • A human intestinal commensal has become a multi-drug resistant pathogen in hospitals, prompting renewed interest in bacteriophages as potential therapies.
  • Despite their promise, the mechanisms of how phages interact with this pathogen and develop resistance are not fully understood.
  • Research shows that phage resistance involves various cell wall molecules and can actually increase susceptibility to certain antibiotics, suggesting that phages could be effective in combination with traditional drugs to combat infections.

Article Abstract

, a commensal of the human intestine, has emerged as a hospital-adapted, multi-drug resistant (MDR) pathogen. Bacteriophages (phages), natural predators of bacteria, have regained attention as therapeutics to stem the rise of MDR bacteria. Despite their potential to curtail MDR infections, the molecular events governing -phage interactions remain largely unknown. Such interactions are important to delineate because phage selective pressure imposed on will undoubtedly result in phage resistance phenotypes that could threaten the efficacy of phage therapy. In an effort to understand the emergence of phage resistance in , three newly isolated lytic phages were used to demonstrate that phage resistance is conferred through an array of cell wall-associated molecules, including secreted antigen A (SagA), enterococcal polysaccharide antigen (Epa), wall teichoic acids, capsule, and an arginine-aspartate-aspartate (RDD) protein of unknown function. We find that capsule and Epa are important for robust phage adsorption and that phage resistance mutations in , , and enhance susceptibility to ceftriaxone, an antibiotic normally ineffective due to its low affinity for enterococcal penicillin binding proteins. Consistent with these findings, we provide evidence that phages potently synergize with cell wall (ceftriaxone and ampicillin) and membrane-acting (daptomycin) antimicrobials to slow or completely inhibit the growth of Our work demonstrates that the evolution of phage resistance comes with fitness defects resulting in drug sensitization and that lytic phages could serve as effective antimicrobials for the treatment of infections.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8092871PMC
http://dx.doi.org/10.1128/AAC.00143-21DOI Listing

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