Publication | Open Access
Discovery and Characterization of QPT-1, the Progenitor of a New Class of Bacterial Topoisomerase Inhibitors
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References
2008
Year
Bioorganic ChemistryMolecular BiologyCompound LibraryAntimicrobial ChemotherapyPharmaceutical ChemistryDrug ResistanceMedicinal ChemistryAntimicrobial ResistanceUnusual Barbituric AcidBacterial Type IiAntibacterial AgentAntimicrobial CompoundMolecular MicrobiologyPharmacologyNatural SciencesRational Drug DesignNew ClassMicrobiologyBacterial Topoisomerase InhibitorsMedicineDrug Discovery
QPT-1 was discovered in a compound library by high-throughput screening and triage for substances with whole-cell antibacterial activity. This totally synthetic compound is an unusual barbituric acid derivative whose activity resides in the (-)-enantiomer. QPT-1 had activity against a broad spectrum of pathogenic, antibiotic-resistant bacteria, was nontoxic to eukaryotic cells, and showed oral efficacy in a murine infection model, all before any medicinal chemistry optimization. Biochemical and genetic characterization showed that the QPT-1 targets the beta subunit of bacterial type II topoisomerases via a mechanism of inhibition distinct from the mechanisms of fluoroquinolones and novobiocin. Given these attributes, this compound represents a promising new class of antibacterial agents. The success of this reverse genomics effort demonstrates the utility of exploring strategies that are alternatives to target-based screens in antibacterial drug discovery.
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