Bismuth antimicrobial drugs serve as broad-spectrum metallo-β-lactamase inhibitors

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作者
Runming Wang
Tsz-Pui Lai
Peng Gao
Hongmin Zhang
Pak-Leung Ho
Patrick Chiu-Yat Woo
Guixing Ma
Richard Yi-Tsun Kao
Hongyan Li
Hongzhe Sun
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[1] The University of Hong Kong,Department of Chemistry
[2] The University of Hong Kong,Department of Microbiology
[3] The University of Hong Kong,The Research Centre of Infection and Immunology, Li Ka Shing Faculty of Medicine
[4] Southern University of Science and Technology,Department of Biology, Guangdong Provincial Key Laboratory of Cell Microenvironment and Disease Research, Shenzhen Key Laboratory of Cell Microenvironment
[5] The University of Hong Kong,State Key Laboratory of Emerging Infectious Diseases
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Drug-resistant superbugs pose a huge threat to human health. Infections by Enterobacteriaceae producing metallo-β-lactamases (MBLs), e.g., New Delhi metallo-β-lactamase 1 (NDM-1) are very difficult to treat. Development of effective MBL inhibitors to revive the efficacy of existing antibiotics is highly desirable. However, such inhibitors are not clinically available till now. Here we show that an anti-Helicobacter pylori drug, colloidal bismuth subcitrate (CBS), and related Bi(III) compounds irreversibly inhibit different types of MBLs via the mechanism, with one Bi(III) displacing two Zn(II) ions as revealed by X-ray crystallography, leading to the release of Zn(II) cofactors. CBS restores meropenem (MER) efficacy against MBL-positive bacteria in vitro, and in mice infection model, importantly, also slows down the development of higher-level resistance in NDM-1-positive bacteria. This study demonstrates a high potential of Bi(III) compounds as the first broad-spectrum B1 MBL inhibitors to treat MBL-positive bacterial infection in conjunction with existing carbapenems.
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