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Membrane Potential-Dependent Uptake of Cationic Oligoimidazolium Mediates Bacterial DNA Damage and Death

The treatment of bacterial infections is becoming increasingly challenging with the emergence of antimicrobial resistance. Thus, the development of antimicrobials with novel mechanisms of action is much needed. Previously, we designed several cationic main-chain imidazolium compounds and identified...

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Autores principales: Yong, Melvin, Kok, Zhi Y., Koh, Chong H., Zhong, Wenbin, Ng, Justin TY., Mu, Yuguang, Chan-Park, Mary B., Gan, Yunn-Hwen
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10190574/
https://www.ncbi.nlm.nih.gov/pubmed/37125913
http://dx.doi.org/10.1128/aac.00355-23
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author Yong, Melvin
Kok, Zhi Y.
Koh, Chong H.
Zhong, Wenbin
Ng, Justin TY.
Mu, Yuguang
Chan-Park, Mary B.
Gan, Yunn-Hwen
author_facet Yong, Melvin
Kok, Zhi Y.
Koh, Chong H.
Zhong, Wenbin
Ng, Justin TY.
Mu, Yuguang
Chan-Park, Mary B.
Gan, Yunn-Hwen
author_sort Yong, Melvin
collection PubMed
description The treatment of bacterial infections is becoming increasingly challenging with the emergence of antimicrobial resistance. Thus, the development of antimicrobials with novel mechanisms of action is much needed. Previously, we designed several cationic main-chain imidazolium compounds and identified the polyimidazolium PIM1 as a potent antibacterial against a wide panel of multidrug-resistant nosocomial pathogens, and it had relatively low toxicity against mammalian epithelial cells. However, little is known about the mechanism of action of PIM1. Using an oligomeric version of PIM1 with precisely six repeating units (OIM1-6) to control for consistency, we showed that OIM1-6 relies on an intact membrane potential for entry into the bacterial cytoplasm, as resistant mutants to OIM1-6 have mutations in their electron transport chains. These mutants demonstrate reduced uptake of the compound, which can be circumvented through the addition of a sub-MIC dose of colistin. Once taken up intracellularly, OIM1-6 exerts double-stranded DNA breaks. Its potency and ability to kill represents a promising class of drugs that can be combined with membrane-penetrating drugs to potentiate activity and hedge against the rise of resistant mutants. In summary, we discovered that cationic antimicrobial OIM1-6 exhibits an antimicrobial property that is dissimilar to the conventional cationic antimicrobial compounds. Its killing mechanism does not involve membrane disruption but instead depends on the membrane potential for uptake into bacterial cells so that it can exert its antibacterial effect intracellularly.
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spelling pubmed-101905742023-05-18 Membrane Potential-Dependent Uptake of Cationic Oligoimidazolium Mediates Bacterial DNA Damage and Death Yong, Melvin Kok, Zhi Y. Koh, Chong H. Zhong, Wenbin Ng, Justin TY. Mu, Yuguang Chan-Park, Mary B. Gan, Yunn-Hwen Antimicrob Agents Chemother Experimental Therapeutics The treatment of bacterial infections is becoming increasingly challenging with the emergence of antimicrobial resistance. Thus, the development of antimicrobials with novel mechanisms of action is much needed. Previously, we designed several cationic main-chain imidazolium compounds and identified the polyimidazolium PIM1 as a potent antibacterial against a wide panel of multidrug-resistant nosocomial pathogens, and it had relatively low toxicity against mammalian epithelial cells. However, little is known about the mechanism of action of PIM1. Using an oligomeric version of PIM1 with precisely six repeating units (OIM1-6) to control for consistency, we showed that OIM1-6 relies on an intact membrane potential for entry into the bacterial cytoplasm, as resistant mutants to OIM1-6 have mutations in their electron transport chains. These mutants demonstrate reduced uptake of the compound, which can be circumvented through the addition of a sub-MIC dose of colistin. Once taken up intracellularly, OIM1-6 exerts double-stranded DNA breaks. Its potency and ability to kill represents a promising class of drugs that can be combined with membrane-penetrating drugs to potentiate activity and hedge against the rise of resistant mutants. In summary, we discovered that cationic antimicrobial OIM1-6 exhibits an antimicrobial property that is dissimilar to the conventional cationic antimicrobial compounds. Its killing mechanism does not involve membrane disruption but instead depends on the membrane potential for uptake into bacterial cells so that it can exert its antibacterial effect intracellularly. American Society for Microbiology 2023-05-01 /pmc/articles/PMC10190574/ /pubmed/37125913 http://dx.doi.org/10.1128/aac.00355-23 Text en Copyright © 2023 Yong et al. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Experimental Therapeutics
Yong, Melvin
Kok, Zhi Y.
Koh, Chong H.
Zhong, Wenbin
Ng, Justin TY.
Mu, Yuguang
Chan-Park, Mary B.
Gan, Yunn-Hwen
Membrane Potential-Dependent Uptake of Cationic Oligoimidazolium Mediates Bacterial DNA Damage and Death
title Membrane Potential-Dependent Uptake of Cationic Oligoimidazolium Mediates Bacterial DNA Damage and Death
title_full Membrane Potential-Dependent Uptake of Cationic Oligoimidazolium Mediates Bacterial DNA Damage and Death
title_fullStr Membrane Potential-Dependent Uptake of Cationic Oligoimidazolium Mediates Bacterial DNA Damage and Death
title_full_unstemmed Membrane Potential-Dependent Uptake of Cationic Oligoimidazolium Mediates Bacterial DNA Damage and Death
title_short Membrane Potential-Dependent Uptake of Cationic Oligoimidazolium Mediates Bacterial DNA Damage and Death
title_sort membrane potential-dependent uptake of cationic oligoimidazolium mediates bacterial dna damage and death
topic Experimental Therapeutics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10190574/
https://www.ncbi.nlm.nih.gov/pubmed/37125913
http://dx.doi.org/10.1128/aac.00355-23
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