Issue 32, 2018, Issue in Progress

Chloramphenicol-borate/boronate complex for controlling infections by chloramphenicol-resistant bacteria

Abstract

Increasing bacterial resistance to antibiotics is a pressing problem worldwide, with many health organisations prioritizing this issue. Whilst there is a desperate need for new effective antimicrobials, it is also important to understand the mechanisms and epidemiology of the resistant pathogens currently present in the community. Chloramphenicol is one such well known antibiotic which had lost its efficacy due to bacterial resistance. In this paper, we report the design, synthesis, and bio-studies of novel chloramphenicol-borate/boronate derivatives which showed the ability to control the infections caused by chloramphenicol-resistant bacteria. Activity profiling against P. aeruginosa strain EXR1 with catB gene indicated the inability of acetyl transferase to acetylate the chloramphenicol-borate/boronate complex, unlike chloramphenicol. Results obtained from the antimicrobial assays were further rationalized by molecular docking studies. The latter revealed that the probable reason for the enhanced antibacterial activity may be attributed to the change in the binding site of chloramphenicol-borate/boronate with chloramphenicol acetyl transferase (CAT) with respect to chloramphenicol itself. Hemolytic and genotoxic studies established the reduced toxicity of these synthetic derivatives with respect to chloramphenicol.

Graphical abstract: Chloramphenicol-borate/boronate complex for controlling infections by chloramphenicol-resistant bacteria

Supplementary files

Article information

Article type
Paper
Submitted
14 Mar 2018
Accepted
06 May 2018
First published
16 May 2018
This article is Open Access
Creative Commons BY-NC license

RSC Adv., 2018,8, 18016-18022

Chloramphenicol-borate/boronate complex for controlling infections by chloramphenicol-resistant bacteria

P. Bhattacharya, M. Singha, K. Senapati, S. Saha, S. Mandal, S. M. Mandal, A. K. Ghosh and A. Basak, RSC Adv., 2018, 8, 18016 DOI: 10.1039/C8RA02227E

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