Literature DB >> 12848621

Lipid binding and membrane penetration of polymyxin B derivatives studied in a biomimetic vesicle system.

Marina Katz1, Haim Tsubery, Sofiya Kolusheva, Alex Shames, Mati Fridkin, Raz Jelinek.   

Abstract

Understanding membrane interactions and cell-wall permeation of Gram-negative bacteria is of great importance, owing to increasing bacterial resistance to existing drugs and therapeutic treatments. Here we use biomimetic lipid vesicles to analyse membrane association and penetration by synthetic derivatives of polymyxin B (PMB), a potent naturally occurring antibacterial cyclic peptide. The PMB analogues studied were PMB nonapeptide (PMBN), in which the hydrophobic alkyl residue was cleaved, PMBN diastereomer containing D-instead of L-amino acids within the cyclic ring (dPMBN) and PMBN where the hydrophobic alkyl chain was replaced with an Ala6 repeat (Ala6-PMBN). Peptide binding measurements, colorimetric transitions induced within the vesicles, fluorescence quenching experiments and ESR spectroscopy were applied to investigate the structural parameters underlying the different membrane-permeation profiles and biological activities of the analogues. The experiments point to the role of negatively charged lipids in membrane binding and confirm the prominence of lipopolisaccharide (LPS) in promoting membrane association and penetration by the peptides. Examination of the lipid interactions of the PMB derivatives shows that the cyclic moiety of PMB is not only implicated in lipid attachment and LPS binding, but also affects penetration into the inner bilayer core. The addition of the Ala6 peptide moiety, however, does not significantly promote peptide insertion into the hydrophobic lipid environment. The data also indicate that the extent of penetration into the lipid bilayer is not related to the overall affinity of the peptides to the membrane.

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Year:  2003        PMID: 12848621      PMCID: PMC1223683          DOI: 10.1042/BJ20030784

Source DB:  PubMed          Journal:  Biochem J        ISSN: 0264-6021            Impact factor:   3.857


  27 in total

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Journal:  Peptides       Date:  2001-10       Impact factor: 3.750

3.  The functional association of polymyxin B with bacterial lipopolysaccharide is stereospecific: studies on polymyxin B nonapeptide.

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4.  A colorimetric assay for rapid screening of antimicrobial peptides.

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5.  Direct colorimetric detection of a receptor-ligand interaction by a polymerized bilayer assembly.

Authors:  D H Charych; J O Nagy; W Spevak; M D Bednarski
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6.  A new colorimetric assay for studying and rapid screening of membrane penetration enhancers.

Authors:  D Evrard; E Touitou; S Kolusheva; Y Fishov; R Jelinek
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7.  Peptide-membrane interactions studied by a new phospholipid/polydiacetylene colorimetric vesicle assay.

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8.  Interactions of mouse Paneth cell alpha-defensins and alpha-defensin precursors with membranes. Prosegment inhibition of peptide association with biomimetic membranes.

Authors:  Donald P Satchell; Tanya Sheynis; Yoshinori Shirafuji; Sofiya Kolusheva; Andre J Ouellette; Raz Jelinek
Journal:  J Biol Chem       Date:  2003-02-06       Impact factor: 5.157

9.  Biomimetic lipid/polymer colorimetric membranes: molecular and cooperative properties.

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10.  Modulation of the hydrophobic domain of polymyxin B nonapeptide: effect on outer-membrane permeabilization and lipopolysaccharide neutralization.

Authors:  Haim Tsubery; Itzhak Ofek; Sofia Cohen; Miriam Eisenstein; Mati Fridkin
Journal:  Mol Pharmacol       Date:  2002-11       Impact factor: 4.436

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  17 in total

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2.  Lipid-Bilayer Dynamics Probed by a Carbon Dot-Phospholipid Conjugate.

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5.  Colorimetric polymer assay for the diagnosis of plasma lipids atherogenic quality in hypercholesterolemic patients.

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Journal:  Antimicrob Agents Chemother       Date:  2006-04       Impact factor: 5.191

7.  Modeling the electrostatic potential of asymmetric lipopolysaccharide membranes: the MEMPOT algorithm implemented in DelPhi.

Authors:  Roberta P Dias; Lin Lin; Thereza A Soares; Emil Alexov
Journal:  J Comput Chem       Date:  2014-05-06       Impact factor: 3.376

8.  Cationic antimicrobial peptides disrupt the Streptococcus pyogenes ExPortal.

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Journal:  Mol Microbiol       Date:  2012-07-26       Impact factor: 3.501

9.  Naturally produced outer membrane vesicles from Pseudomonas aeruginosa elicit a potent innate immune response via combined sensing of both lipopolysaccharide and protein components.

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10.  Disruption of Membrane by Colistin Kills Uropathogenic Escherichia coli Persisters and Enhances Killing of Other Antibiotics.

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