Molecules (Jun 2022)

Recent Developments to Cope the Antibacterial Resistance via β-Lactamase Inhibition

  • Zafar Iqbal,
  • Jian Sun,
  • Haikang Yang,
  • Jingwen Ji,
  • Lili He,
  • Lijuan Zhai,
  • Jinbo Ji,
  • Pengjuan Zhou,
  • Dong Tang,
  • Yangxiu Mu,
  • Lin Wang,
  • Zhixiang Yang

DOI
https://doi.org/10.3390/molecules27123832
Journal volume & issue
Vol. 27, no. 12
p. 3832

Abstract

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Antibacterial resistance towards the β-lactam (BL) drugs is now ubiquitous, and there is a major global health concern associated with the emergence of new β-lactamases (BLAs) as the primary cause of resistance. In addition to the development of new antibacterial drugs, β-lactamase inhibition is an alternative modality that can be implemented to tackle this resistance channel. This strategy has successfully revitalized the efficacy of a number of otherwise obsolete BLs since the discovery of the first β-lactamase inhibitor (BLI), clavulanic acid. Over the years, β-lactamase inhibition research has grown, leading to the introduction of new synthetic inhibitors, and a few are currently in clinical trials. Of note, the 1, 6-diazabicyclo [3,2,1]octan-7-one (DBO) scaffold gained the attention of researchers around the world, which finally culminated in the approval of two BLIs, avibactam and relebactam, which can successfully inhibit Ambler class A, C, and D β-lactamases. Boronic acids have shown promise in coping with Ambler class B β-lactamases in recent research, in addition to classes A, C, and D with the clinical use of vaborbactam. This review focuses on the further developments in the synthetic strategies using DBO as well as boronic acid derivatives. In addition, various other potential serine- and metallo- β-lactamases inhibitors that have been developed in last few years are discussed briefly as well. Furthermore, binding interactions of the representative inhibitors have been discussed based on the crystal structure data of inhibitor-enzyme complex, published in the literature.

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