2024
DOI: 10.1021/acsinfecdis.3c00346
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Interactions between Gepotidacin and Escherichia coli Gyrase and Topoisomerase IV: Genetic and Biochemical Evidence for Well-Balanced Dual-Targeting

Alexandria A. Oviatt,
Elizabeth G. Gibson,
Jianzhong Huang
et al.

Abstract: Antimicrobial resistance is a global threat to human health. Therefore, efforts have been made to develop new antibacterial agents that address this critical medical issue. Gepotidacin is a novel, bactericidal, first-in-class triazaacenaphthylene antibacterial in clinical development. Recently, phase III clinical trials for gepotidacin treatment of uncomplicated urinary tract infections caused by uropathogens, including Escherichia coli, were stopped for demonstrated efficacy. Because of the clinical promise o… Show more

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Cited by 7 publications
(14 citation statements)
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“…The NBTI LHS sits in a pocket in the DNA on the 2-fold axis of the complex, midway between the two DNA cleavage sites, and the RHS sits in a pocket on the 2-fold axis between the two GyrA subunits. ,,, One of the most important interactions between gyrase/topoisomerase IV and the NBTI is with an aspartic acid residue (Asp82 in E. coli GyrA), which forms a hydrogen bond with the basic nitrogen. NBTIs do not interact directly with the serine or acidic residues that are critical for fluoroquinolone binding. ,,, Even though the binding sites of fluoroquinolones and NBTIs do not overlap, it appears that both drugs cannot bind to the active site of gyrase/topoisomerase IV simultaneously. ,, …”
Section: Novel Bacterial Topoisomerase Inhibitors M Tuberculosis Gyra...mentioning
confidence: 99%
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“…The NBTI LHS sits in a pocket in the DNA on the 2-fold axis of the complex, midway between the two DNA cleavage sites, and the RHS sits in a pocket on the 2-fold axis between the two GyrA subunits. ,,, One of the most important interactions between gyrase/topoisomerase IV and the NBTI is with an aspartic acid residue (Asp82 in E. coli GyrA), which forms a hydrogen bond with the basic nitrogen. NBTIs do not interact directly with the serine or acidic residues that are critical for fluoroquinolone binding. ,,, Even though the binding sites of fluoroquinolones and NBTIs do not overlap, it appears that both drugs cannot bind to the active site of gyrase/topoisomerase IV simultaneously. ,, …”
Section: Novel Bacterial Topoisomerase Inhibitors M Tuberculosis Gyra...mentioning
confidence: 99%
“…Because of the recent emergence of NBTIs as an antibacterial class with clinical potential, relatively little is known about resistance. However, mutations in gyrase/topoisomerase IV that decrease the sensitivity of laboratory strains and clinical isolates to this drug class have been reported. ,, A prominent mutation occurs at the aspartic acid residue that has been shown to interact with NBTIs in structural studies. ,, The response of NBTIs to fluoroquinolone resistance mutations varies across compounds and species. Whereas moderate to high levels of resistance are observed in some drug-species combinations, in others, such as MGIs and M. tuberculosis gyrase, compounds are more potent and efficacious against enzymes that carry a fluoroquinolone resistance mutation. ,,,,, …”
Section: Novel Bacterial Topoisomerase Inhibitors M Tuberculosis Gyra...mentioning
confidence: 99%
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