Literature DB >> 22700968

Progressive structuring of a branched antimicrobial peptide on the path to the inner membrane target.

Yang Bai1, Shouping Liu, Jianguo Li, Rajamani Lakshminarayanan, Padmanabhan Sarawathi, Charles Tang, Duncun Ho, Chandra Verma, Roger W Beuerman, Konstantin Pervushin.   

Abstract

In recent years, interest has grown in the antimicrobial properties of certain natural and non-natural peptides. The strategy of inserting a covalent branch point in a peptide can improve its antimicrobial properties while retaining host biocompatibility. However, little is known regarding possible structural transitions as the peptide moves on the access path to the presumed target, the inner membrane. Establishing the nature of the interactions with the complex bacterial outer and inner membranes is important for effective peptide design. Structure-activity relationships of an amphiphilic, branched antimicrobial peptide (B2088) are examined using environment-sensitive fluorescent probes, electron microscopy, molecular dynamics simulations, and high resolution NMR in solution and in condensed states. The peptide is reconstituted in bacterial outer membrane lipopolysaccharide extract as well as in a variety of lipid media mimicking the inner membrane of Gram-negative pathogens. Progressive structure accretion is observed for the peptide in water, LPS, and lipid environments. Despite inducing rapid aggregation of bacteria-derived lipopolysaccharides, the peptide remains highly mobile in the aggregated lattice. At the inner membranes, the peptide undergoes further structural compaction mediated by interactions with negatively charged lipids, probably causing redistribution of membrane lipids, which in turn results in increased membrane permeability and bacterial lysis. These findings suggest that peptides possessing both enhanced mobility in the bacterial outer membrane and spatial structure facilitating its interactions with the membrane-water interface may provide excellent structural motifs to develop new antimicrobials that can overcome antibiotic-resistant Gram-negative pathogens.

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Year:  2012        PMID: 22700968      PMCID: PMC3411001          DOI: 10.1074/jbc.M112.363259

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  78 in total

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10.  Structure-dependent charge density as a determinant of antimicrobial activity of peptide analogues of defensin.

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2.  Dimeric unnatural polyproline-rich peptides with enhanced antibacterial activity.

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3.  Antimicrobial Peptides: Insights into Membrane Permeabilization, Lipopolysaccharide Fragmentation and Application in Plant Disease Control.

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4.  Branched Peptide, B2088, Disrupts the Supramolecular Organization of Lipopolysaccharides and Sensitizes the Gram-negative Bacteria.

Authors:  Rajamani Lakshminarayanan; Wei Xiang Tan; Thet Tun Aung; Eunice Tze Leng Goh; Nandhakumar Muruganantham; Jianguo Li; Jamie Ya Ting Chang; Neha Dikshit; Padmanabhan Saraswathi; Rayne Rui Lim; Tse Siang Kang; Vanniarajan Balamuralidhar; Bindu Sukumaran; Chandra S Verma; Jayaraman Sivaraman; Shyam Sunder Chaurasia; Shouping Liu; Roger W Beuerman
Journal:  Sci Rep       Date:  2016-05-13       Impact factor: 4.379

Review 5.  Membrane Active Antimicrobial Peptides: Translating Mechanistic Insights to Design.

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  5 in total

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