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Resensitizing carbapenem- and colistin-resistant bacteria to antibiotics using auranofin

Medicine and Health

Resensitizing carbapenem- and colistin-resistant bacteria to antibiotics using auranofin

H. Sun, Q. Zhang, et al.

The emergence of Gram-negative bacteria with resistance genes presents a daunting challenge in infection treatment. This study by Hongzhe Sun and colleagues reveals auranofin as a promising dual inhibitor against metallo-β-lactamases and mobilized colistin resistance, potentially transforming therapeutic strategies in combating resistant infections.

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~3 min • Beginner • English
Abstract
Global emergence of Gram-negative bacteria carrying plasmid-borne resistance genes, including blaMBL and mcr, challenges the treatment of life-threatening infections with carbapenems and colistin. This study identifies the antirheumatic drug auranofin (AUR) as a dual inhibitor of metallo-β-lactamases (MBLs) and mobilized colistin resistance enzymes (MCRs), which have distinct structures and substrates. AUR irreversibly abrogates both enzyme activities by displacing Zn(II) cofactors from their active sites. AUR synergizes with antibiotics to kill a broad spectrum of carbapenem- and/or colistin-resistant bacteria and slows the development of β-lactam and colistin resistance. Combination of AUR and colistin rescues all mice infected by Escherichia coli co-expressing MCR-1 and NDM-5. These findings support combining AUR with antibiotics to combat pathogens co-producing MBLs and MCRs.
Publisher
Nature Communications
Published On
Oct 16, 2020
Authors
Hongzhe Sun, Qi Zhang, Runming Wang, Haibo Wang, Yuen-Ting Wong, Minji Wang, Quan Hao, Aixin Yan, Richard Yi-Tsun Kao, Pak-Leung Ho, Hongyan Li
Tags
Gram-negative bacteria
plasmid-borne resistance
auranofin
metallo-β-lactamases
colistin resistance
antibiotic synergy
infection treatment
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