In silico identification of two peptides with antibacterial activity against multidrug-resistant Staphylococcus aureus

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作者
Linda B. Oyama
Hamza Olleik
Ana Carolina Nery Teixeira
Matheus M. Guidini
James A. Pickup
Brandon Yeo Pei Hui
Nicolas Vidal
Alan R. Cookson
Hannah Vallin
Toby Wilkinson
Denise M. S. Bazzolli
Jennifer Richards
Mandy Wootton
Ralf Mikut
Kai Hilpert
Marc Maresca
Josette Perrier
Matthias Hess
Hilario C. Mantovani
Narcis Fernandez-Fuentes
Christopher J. Creevey
Sharon A. Huws
机构
[1] Queen’s University Belfast,Institute for Global Food Security, School of Biological Sciences
[2] Université de Technologie de Compiègne,CNRS Enzyme and Cell Engineering Laboratory
[3] Sorbonne Universités,Departamento de Microbiologia
[4] Universidade Federal de Viçosa,Yelen Analytics
[5] University College Fairview (UCF),Institute of Biological Environmental and Rural Sciences
[6] Aix-Marseille University ICR,The Roslin Institute and R(D)SVS
[7] Aberystwyth University,Specialist Antimicrobial Chemotherapy Unit, Public Health Wales
[8] University of Edinburgh,Karlsruhe Institute of Technology
[9] University Hospital of Wales,Institute of Infection and Immunity, St George’s
[10] Heath Park,undefined
[11] Institute for Automation and Applied Informatics,undefined
[12] University of London,undefined
[13] Cranmer Terrace,undefined
[14] Aix Marseille University,undefined
[15] UC Davis,undefined
[16] College of Agricultural and Environmental Sciences,undefined
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摘要
Here we report two antimicrobial peptides (AMPs), HG2 and HG4 identified from a rumen microbiome metagenomic dataset, with activity against multidrug-resistant (MDR) bacteria, especially methicillin-resistant Staphylococcus aureus (MRSA) strains, a major hospital and community-acquired pathogen. We employed the classifier model design to analyse, visualise, and interpret AMP activities. This approach allowed in silico discrimination of promising lead AMP candidates for experimental evaluation. The lead AMPs, HG2 and HG4, are fast-acting and show anti-biofilm and anti-inflammatory activities in vitro and demonstrated little toxicity to human primary cell lines. The peptides were effective in vivo within a Galleria mellonella model of MRSA USA300 infection. In terms of mechanism of action, HG2 and HG4 appear to interact with the cytoplasmic membrane of target cells and may inhibit other cellular processes, whilst preferentially binding to bacterial lipids over human cell lipids. Therefore, these AMPs may offer additional therapeutic templates for MDR bacterial infections.
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