Literature DB >> 24743021

Two interdependent mechanisms of antimicrobial activity allow for efficient killing in nylon-3-based polymeric mimics of innate immunity peptides.

Michelle W Lee1, Saswata Chakraborty2, Nathan W Schmidt1, Rajan Murgai1, Samuel H Gellman2, Gerard C L Wong3.   

Abstract

Novel synthetic mimics of antimicrobial peptides have been developed to exhibit structural properties and antimicrobial activity similar to those of natural antimicrobial peptides (AMPs) of the innate immune system. These molecules have a number of potential advantages over conventional antibiotics, including reduced bacterial resistance, cost-effective preparation, and customizable designs. In this study, we investigate a family of nylon-3 polymer-based antimicrobials. By combining vesicle dye leakage, bacterial permeation, and bactericidal assays with small-angle X-ray scattering (SAXS), we find that these polymers are capable of two interdependent mechanisms of action: permeation of bacterial membranes and binding to intracellular targets such as DNA, with the latter necessarily dependent on the former. We systemically examine polymer-induced membrane deformation modes across a range of lipid compositions that mimic both bacteria and mammalian cell membranes. The results show that the polymers' ability to generate negative Gaussian curvature (NGC), a topological requirement for membrane permeation and cellular entry, in model Escherichia coli membranes correlates with their ability to permeate membranes without complete membrane disruption and kill E. coli cells. Our findings suggest that these polymers operate with a concentration-dependent mechanism of action: at low concentrations permeation and DNA binding occur without membrane disruption, while at high concentrations complete disruption of the membrane occurs. This article is part of a Special Issue entitled: Interfacially Active Peptides and Proteins. Guest Editors: William C. Wimley and Kalina Hristova.
Copyright © 2014 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  antimicrobial peptides; innate immunity; membrane curvature; membrane permeation; peptide–lipid interactions; pore formation

Mesh:

Substances:

Year:  2014        PMID: 24743021      PMCID: PMC4405380          DOI: 10.1016/j.bbamem.2014.04.007

Source DB:  PubMed          Journal:  Biochim Biophys Acta        ISSN: 0006-3002


  88 in total

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3.  Inverse lyotropic phases of lipids and membrane curvature.

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4.  Small-angle X-ray scattering studies of peptide-lipid interactions using the mouse paneth cell α-defensin cryptdin-4.

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5.  Alteration of the phospholipid composition of Staphylococcus aureus cultured in medium containing NaCl.

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6.  Chromosomal location of genes regulating resistance to bacteriophage in Bacillus subtilis.

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  12 in total

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3.  Direct Antimicrobial Activity of IFN-β.

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4.  Histidine-Mediated Ion Specific Effects Enable Salt Tolerance of a Pore-Forming Marine Antimicrobial Peptide.

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Review 5.  Machine learning-enabled discovery and design of membrane-active peptides.

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6.  Single-Cell, Time-Resolved Antimicrobial Effects of a Highly Cationic, Random Nylon-3 Copolymer on Live Escherichia coli.

Authors:  Heejun Choi; Saswata Chakraborty; Runhui Liu; Samuel H Gellman; James C Weisshaar
Journal:  ACS Chem Biol       Date:  2015-11-05       Impact factor: 5.100

Review 7.  What Can Pleiotropic Proteins in Innate Immunity Teach Us about Bioconjugation and Molecular Design?

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8.  How do cyclic antibiotics with activity against Gram-negative bacteria permeate membranes? A machine learning informed experimental study.

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9.  Molecular Motor Dnm1 Synergistically Induces Membrane Curvature To Facilitate Mitochondrial Fission.

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10.  Switchable Membrane Remodeling and Antifungal Defense by Metamorphic Chemokine XCL1.

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