Publication | Closed Access
Zinc Chelation by a Small-Molecule Adjuvant Potentiates Meropenem Activity in Vivo against NDM-1-Producing <i>Klebsiella pneumoniae</i>
55
Citations
27
References
2015
Year
Antimicrobial ChemotherapyAntibiotic ResistanceDrug ResistanceAntibiotic Drug ResistanceAntimicrobial TherapyBiological Inorganic ChemistryAntimicrobial ResistanceAntimicrobial Drug DiscoveryDrug Resistance AnalysisBiochemistryAntibacterial AgentAntimicrobial PharmacokineticsAntimicrobial CompoundPharmacologyWidespread EmergenceAntibioticsZinc ChelationNatural SciencesBioactive MetalMicrobiologyAntimicrobial PharmacodynamicsMedicineSmall MoleculesDrug Discovery
The widespread emergence of antibiotic drug resistance has resulted in a worldwide healthcare crisis. In particular, the extensive use of β-lactams, a highly effective class of antibiotics, has been a driver for pervasive β-lactam resistance. Among the most important resistance determinants are the metallo-β-lactamases (MBL), which are zinc-requiring enzymes that inactivate nearly all classes of β-lactams, including the last-resort carbapenem antibiotics. The urgent need for new compounds targeting MBL resistance mechanisms has been widely acknowledged; however, the development of certain types of compounds-namely metal chelators-is actively avoided due to host toxicity concerns. The work herein reports the identification of a series of zinc-selective spiro-indoline-thiadiazole analogues that, in vitro, potentiate β-lactam antibiotics against an MBL-carrying pathogen by withholding zinc availability. This study demonstrates the ability of one such analogue to inhibit NDM-1 in vitro and, using a mouse model of infection, shows that combination treatment of the respective analogue with meropenem results in a significant decrease in bacterial burden in contrast to animals that received antibiotic treatment alone. These results support the therapeutic potential of these chelators in overcoming antibiotic resistance.
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