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Systematic comparison of activity and mechanism of antimicrobial peptides against nosocomial pathogens

Authors :
Lin, B
Hung, A
Li, R
Barlow, A
Singleton, W
Matthyssen, T
Sani, M-AD
Hossain, MA
Wade, J
O'Brien-Simpson, NM
Li, W
Lin, B
Hung, A
Li, R
Barlow, A
Singleton, W
Matthyssen, T
Sani, M-AD
Hossain, MA
Wade, J
O'Brien-Simpson, NM
Li, W
Publication Year :
2022

Abstract

The World Health Organisation has deemed several multi-drug resistant (MDR) nosocomial bacterial pathogens to be of significant threat to human health. A stark increase in morbidity, mortality and the burden to healthcare systems around the world can be attributed to the development of resistance in these bacteria. Accordingly, alternative antimicrobial agents have been sought as an attractive means to combat MDR pathogens, with one such example being antimicrobial peptides (AMPs). Given the reported activity of AMPs, including Pardaxin, MSI-78, dermaseptin-PC (DMPC) and Cecropin B, it is important to understand their activities and modes of action against bacteria for further AMP design. In this study, we compared these AMPs against a panel of nosocomial bacterial pathogens, followed by detailed mechanistic studies. It was found that Pardaxin (1-22) and MSI-78 (4-20) displayed the most pronounced antimicrobial activity against the tested bacteria. The mechanistic studies by membrane permeability and molecular dynamics simulation further confirmed the strong membrane interaction and structure of Pardaxin (1-22) and MSI-78 (4-20), which contributed to their potent activity. This study demonstrated a structure and activity guidance for further design of Pardaxin (1-22) and MSI-78 (4-20) as therapeutics against MDR pathogens. The different effects of DMPC (1-19) and Cecropin B (1-21) on membrane integrity and phospholipid membrane interactions provided critical information for the rational design of next-generation analogues with specificity against either Gram-negative or Gram-positive bacteria.

Details

Database :
OAIster
Publication Type :
Electronic Resource
Accession number :
edsoai.on1397539158
Document Type :
Electronic Resource