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

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

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...

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Main Authors: Beuerman, Roger W., Bai, Yang, Liu, Shouping, Li, Jianguo, Lakshminarayanan, Rajamani, Sarawathi, Padmanabhan, Tang, Charles, Ho, Duncun, Verma, Chandra, Pervushin, Konstantin
Other Authors: School of Biological Sciences
Format: Article
Language:English
Published: 2013
Subjects:
DRNTU::Science::Biological sciences::Biochemistry
Online Access:https://hdl.handle.net/10356/105331
http://hdl.handle.net/10220/17200
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Institution: Nanyang Technological University
Language: English
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spelling sg-ntu-dr.10356-1053312022-02-16T16:29:07Z Progressive structuring of a branched antimicrobial peptide on the path to the inner membrane target Beuerman, Roger W. Bai, Yang Liu, Shouping Li, Jianguo Lakshminarayanan, Rajamani Sarawathi, Padmanabhan Tang, Charles Ho, Duncun Verma, Chandra Pervushin, Konstantin School of Biological Sciences DRNTU::Science::Biological sciences::Biochemistry 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. 2013-11-01T02:12:12Z 2019-12-06T21:49:17Z 2013-11-01T02:12:12Z 2019-12-06T21:49:17Z 2012 2012 Journal Article Bai, Y., Liu, S., Li, J., Lakshminarayanan, R., Sarawathi, P., Tang, C., et al. (2012). Progressive structuring of a branched antimicrobial peptide on the path to the inner membrane target. Journal of biological chemistry, 287(32), 26606-26617. https://hdl.handle.net/10356/105331 http://hdl.handle.net/10220/17200 10.1074/jbc.M112.363259 22700968 en Journal of biological chemistry
institution Nanyang Technological University
building NTU Library
continent Asia
country Singapore
Singapore
content_provider NTU Library
collection DR-NTU
language English
topic DRNTU::Science::Biological sciences::Biochemistry
spellingShingle DRNTU::Science::Biological sciences::Biochemistry
Beuerman, Roger W.
Bai, Yang
Liu, Shouping
Li, Jianguo
Lakshminarayanan, Rajamani
Sarawathi, Padmanabhan
Tang, Charles
Ho, Duncun
Verma, Chandra
Pervushin, Konstantin
Progressive structuring of a branched antimicrobial peptide on the path to the inner membrane target
description 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.
author2 School of Biological Sciences
author_facet School of Biological Sciences
Beuerman, Roger W.
Bai, Yang
Liu, Shouping
Li, Jianguo
Lakshminarayanan, Rajamani
Sarawathi, Padmanabhan
Tang, Charles
Ho, Duncun
Verma, Chandra
Pervushin, Konstantin
format Article
author Beuerman, Roger W.
Bai, Yang
Liu, Shouping
Li, Jianguo
Lakshminarayanan, Rajamani
Sarawathi, Padmanabhan
Tang, Charles
Ho, Duncun
Verma, Chandra
Pervushin, Konstantin
author_sort Beuerman, Roger W.
title Progressive structuring of a branched antimicrobial peptide on the path to the inner membrane target
title_short Progressive structuring of a branched antimicrobial peptide on the path to the inner membrane target
title_full Progressive structuring of a branched antimicrobial peptide on the path to the inner membrane target
title_fullStr Progressive structuring of a branched antimicrobial peptide on the path to the inner membrane target
title_full_unstemmed Progressive structuring of a branched antimicrobial peptide on the path to the inner membrane target
title_sort progressive structuring of a branched antimicrobial peptide on the path to the inner membrane target
publishDate 2013
url https://hdl.handle.net/10356/105331
http://hdl.handle.net/10220/17200
_version_ 1725985517358546944

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