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Multiform antimicrobial resistance from a metabolic mutation

Authors :
Helene Botella
Carl Nathan
Kyu Y. Rhee
Sarah M. Schrader
Sabine Ehrt
Robert S. Jansen
Julien Vaubourgeix
Commission of the European Communities
Source :
Science Advances, Science Advances, 7, 1-17, Science Advances, 7, 35, pp. 1-17
Publication Year :
2021
Publisher :
American Association for the Advancement of Science, 2021.

Abstract

Disruption of a metabolic pathway causes tolerance, high persistence, and MIC-shifted resistance to diverse antibiotics.<br />A critical challenge for microbiology and medicine is how to cure infections by bacteria that survive antibiotic treatment by persistence or tolerance. Seeking mechanisms behind such high survival, we developed a forward-genetic method for efficient isolation of high-survival mutants in any culturable bacterial species. We found that perturbation of an essential biosynthetic pathway (arginine biosynthesis) in a mycobacterium generated three distinct forms of resistance to diverse antibiotics, each mediated by induction of WhiB7: high persistence and tolerance to kanamycin, high survival upon exposure to rifampicin, and minimum inhibitory concentration–shifted resistance to clarithromycin. As little as one base change in a gene that encodes, a metabolic pathway component conferred multiple forms of resistance to multiple antibiotics with different targets. This extraordinary resilience may help explain how substerilizing exposure to one antibiotic in a regimen can induce resistance to others and invites development of drugs targeting the mediator of multiform resistance, WhiB7.

Details

ISSN :
23752548
Database :
OpenAIRE
Journal :
Science Advances, Science Advances, 7, 1-17, Science Advances, 7, 35, pp. 1-17
Accession number :
edsair.doi.dedup.....5fc9cca1e082da6fd24a79613979e2ce