Literature DB >> 20448930

Synchrotron radiation linear dichroism spectroscopy of the antibiotic peptide gramicidin in lipid membranes.

Matthew R Hicks1, Timothy R Dafforn, Angeliki Damianoglou, Paul Wormell, Alison Rodger, Søren V Hoffmann.   

Abstract

We have developed synchrotron radiation linear dichroism (SRLD) to measure the insertion of peptides into lipid bilayers, significantly improving both signal-to-noise and wavelength range over existing methods. Our wavelength cut-off is currently determined by the quality of quartz in the cell, rather than the light source, with signal quality still high at the cut-off. We demonstrate the use of a lipid probe to measure the orientation of the lipid bilayers under flow and describe the way in which this can be used to further interpret SRLD data. The antibiotic peptide gramicidin is shown to exhibit drastically different kinetic and equilibrium behaviour when interacting with lipid membranes with different properties. The charge on the membrane is of interest because of differences in charge between human and bacterial membranes. For this reason we increased the negative charge on the membrane by changing the lipid composition. Increasing negative charge in the gel phase stabilises the liposomes but changes the kinetics of peptide folding. In a gel phase with no negatively charged lipids, gramicidin does not fold well and gives a small signal that indicates a change in orientation of the tryptophan side chains over time. In the fluid phase with no negatively charged lipids, there is initially >10-fold greater peptide signal relative to the gel phase indicating a highly folded and ordered gramicidin backbone. This is followed by liposome disruption. In the gel phase with negatively charged lipids the liposomes are resistant to disruption by gramicidin and exhibit different folding kinetics depending on membrane composition. In the fluid phase with negatively charged lipids there is little signal from either the peptide or the lipid probe indicating that the liposomes have been disrupted by the gramicidin in the time it takes to make the first measurement.

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Year:  2009        PMID: 20448930     DOI: 10.1039/b902523e

Source DB:  PubMed          Journal:  Analyst        ISSN: 0003-2654            Impact factor:   4.616


  3 in total

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Authors:  Emma L Gilroy; Søren Vrønning Hoffmann; Nykola C Jones; Alison Rodger
Journal:  Eur Biophys J       Date:  2011-09-20       Impact factor: 1.733

2.  Role of liposome and peptide in the synergistic enhancement of transfection with a lipopolyplex vector.

Authors:  Mustafa M Munye; Jascindra Ravi; Aristides D Tagalakis; David McCarthy; Maxim G Ryadnov; Stephen L Hart
Journal:  Sci Rep       Date:  2015-03-19       Impact factor: 4.379

3.  Insight into the Mechanism of Action and Peptide-Membrane Interactions of Aib-Rich Peptides: Multitechnique Experimental and Theoretical Analysis.

Authors:  Maria Giovanna Lizio; Mario Campana; Matteo De Poli; Damien F Jefferies; William Cullen; Valery Andrushchenko; Nikola P Chmel; Petr Bouř; Syma Khalid; Jonathan Clayden; Ewan Blanch; Alison Rodger; Simon J Webb
Journal:  Chembiochem       Date:  2021-02-24       Impact factor: 3.164

  3 in total

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