Potent antibacterial activity of MSI-1 derived from the magainin 2 peptide against drug-resistant bacteria

The structural modification of existing AMPs is an effective strategy to develop antimicrobial agents with high-efficiency, low-cost and low-toxicity antimicrobial agents. Methods: Here, we truncated 14-amino-acids at the N-terminus of MSI-78 to obtain MSI and further modified MSI to obtain four pep...

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Autores principales: Ma, Lingman, Xie, Xin, Liu, Hanhan, Huang, Ya, Wu, Haomin, Jiang, Meiling, Xu, Pengfei, Ye, Xinyue, Zhou, Changlin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2020
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6956804/
https://www.ncbi.nlm.nih.gov/pubmed/31938070
http://dx.doi.org/10.7150/thno.39157
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author Ma, Lingman
Xie, Xin
Liu, Hanhan
Huang, Ya
Wu, Haomin
Jiang, Meiling
Xu, Pengfei
Ye, Xinyue
Zhou, Changlin
author_facet Ma, Lingman
Xie, Xin
Liu, Hanhan
Huang, Ya
Wu, Haomin
Jiang, Meiling
Xu, Pengfei
Ye, Xinyue
Zhou, Changlin
author_sort Ma, Lingman
collection PubMed
description The structural modification of existing AMPs is an effective strategy to develop antimicrobial agents with high-efficiency, low-cost and low-toxicity antimicrobial agents. Methods: Here, we truncated 14-amino-acids at the N-terminus of MSI-78 to obtain MSI and further modified MSI to obtain four peptide analogs: MSI-1, MSI-2, MSI-3 and MSI-4. These peptide mutants were evaluated regarding their antibacterial activity against various sensitive or resistant bacteria; toxicity against mammalian cells or mice; and stability against violent pH, temperature variations and high NaCl concentrations. Finally, we also elucidated the possible mechanisms underlying its mode of action. Results: The results showed that MSI-1 and MSI-3 displayed activity that was superior to that of MSI-78 with MICs of 4-16 μg/ml and MBCs of 8-64 μg/ml, respectively, especially against drug-resistant bacteria, due to the increase in percent helicity and amphiphilicity. However, MSI-3, with higher hydrophobicity and antibacterial activity, had a relatively higher hemolysis rate and toxicity than MSI-1. MSI-1 exerted rapid bactericidal activity and effectively improved the survival rate and wound closure in penicillin-resistant E. coli-infected mice by eliminating bacterial counts in mouse organs or subeschar, further inhibiting the systemic dissemination of bacteria. Additionally, MSI-1 displayed perfect stability against violent pH, temperature variations and high NaCl concentrations and has the ability to circumvent the development of drug resistance. In terms of the mode of action, we found that at the super-MIC level, MSI-1 exhibited direct antimicrobial activity by disrupting the integrity of the bacterial cell membrane, while at the sub-MIC level, it bound to bacterial DNA to inhibit DNA replication and protein expression and ultimately disrupted bacterial biological function. Conclusions: This novel peptide MSI-1 could be a potential candidate for drug development against infection induced by drug-resistant bacteria.
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spelling pubmed-69568042020-01-14 Potent antibacterial activity of MSI-1 derived from the magainin 2 peptide against drug-resistant bacteria Ma, Lingman Xie, Xin Liu, Hanhan Huang, Ya Wu, Haomin Jiang, Meiling Xu, Pengfei Ye, Xinyue Zhou, Changlin Theranostics Research Paper The structural modification of existing AMPs is an effective strategy to develop antimicrobial agents with high-efficiency, low-cost and low-toxicity antimicrobial agents. Methods: Here, we truncated 14-amino-acids at the N-terminus of MSI-78 to obtain MSI and further modified MSI to obtain four peptide analogs: MSI-1, MSI-2, MSI-3 and MSI-4. These peptide mutants were evaluated regarding their antibacterial activity against various sensitive or resistant bacteria; toxicity against mammalian cells or mice; and stability against violent pH, temperature variations and high NaCl concentrations. Finally, we also elucidated the possible mechanisms underlying its mode of action. Results: The results showed that MSI-1 and MSI-3 displayed activity that was superior to that of MSI-78 with MICs of 4-16 μg/ml and MBCs of 8-64 μg/ml, respectively, especially against drug-resistant bacteria, due to the increase in percent helicity and amphiphilicity. However, MSI-3, with higher hydrophobicity and antibacterial activity, had a relatively higher hemolysis rate and toxicity than MSI-1. MSI-1 exerted rapid bactericidal activity and effectively improved the survival rate and wound closure in penicillin-resistant E. coli-infected mice by eliminating bacterial counts in mouse organs or subeschar, further inhibiting the systemic dissemination of bacteria. Additionally, MSI-1 displayed perfect stability against violent pH, temperature variations and high NaCl concentrations and has the ability to circumvent the development of drug resistance. In terms of the mode of action, we found that at the super-MIC level, MSI-1 exhibited direct antimicrobial activity by disrupting the integrity of the bacterial cell membrane, while at the sub-MIC level, it bound to bacterial DNA to inhibit DNA replication and protein expression and ultimately disrupted bacterial biological function. Conclusions: This novel peptide MSI-1 could be a potential candidate for drug development against infection induced by drug-resistant bacteria. Ivyspring International Publisher 2020-01-01 /pmc/articles/PMC6956804/ /pubmed/31938070 http://dx.doi.org/10.7150/thno.39157 Text en © The author(s) This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Ma, Lingman
Xie, Xin
Liu, Hanhan
Huang, Ya
Wu, Haomin
Jiang, Meiling
Xu, Pengfei
Ye, Xinyue
Zhou, Changlin
Potent antibacterial activity of MSI-1 derived from the magainin 2 peptide against drug-resistant bacteria
title Potent antibacterial activity of MSI-1 derived from the magainin 2 peptide against drug-resistant bacteria
title_full Potent antibacterial activity of MSI-1 derived from the magainin 2 peptide against drug-resistant bacteria
title_fullStr Potent antibacterial activity of MSI-1 derived from the magainin 2 peptide against drug-resistant bacteria
title_full_unstemmed Potent antibacterial activity of MSI-1 derived from the magainin 2 peptide against drug-resistant bacteria
title_short Potent antibacterial activity of MSI-1 derived from the magainin 2 peptide against drug-resistant bacteria
title_sort potent antibacterial activity of msi-1 derived from the magainin 2 peptide against drug-resistant bacteria
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6956804/
https://www.ncbi.nlm.nih.gov/pubmed/31938070
http://dx.doi.org/10.7150/thno.39157
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