AI Article Synopsis

  • The rise of drug-resistant tuberculosis has sparked the need for new antibacterial treatments, with a focus on a class of compounds called spiropyrimidinetriones (SPTs) that target bacterial gyrase, similar to fluoroquinolone antibiotics.
  • H3D-005722 and related SPTs showed strong activity in inducing DNA breaks by gyrase, performing comparably to existing antibiotics moxifloxacin and ciprofloxacin, and surpassing the effects of zoliflodacin.
  • Notably, these SPTs were effective against common gyrase mutations that confer resistance to fluoroquinolones, often displaying greater activity against mutant forms than against the wild type, while showing low inhibition of human topoisomerase IIα,

Article Abstract

The rise in drug-resistant tuberculosis has necessitated the search for alternative antibacterial treatments. Spiropyrimidinetriones (SPTs) represent an important new class of compounds that work through gyrase, the cytotoxic target of fluoroquinolone antibacterials. The present study analyzed the effects of a novel series of SPTs on the DNA cleavage activity of gyrase. H3D-005722 and related SPTs displayed high activity against gyrase and increased levels of enzyme-mediated double-stranded DNA breaks. The activities of these compounds were similar to those of the fluoroquinolones, moxifloxacin, and ciprofloxacin and greater than that of zoliflodacin, the most clinically advanced SPT. All the SPTs overcame the most common mutations in gyrase associated with fluoroquinolone resistance and, in most cases, were more active against the mutant enzymes than wild-type gyrase. Finally, the compounds displayed low activity against human topoisomerase IIα. These findings support the potential of novel SPT analogues as antitubercular drugs.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10006343PMC
http://dx.doi.org/10.1021/acsinfecdis.3c00012DOI Listing

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