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Please use this identifier to cite or link to this item: https://doi.org/10.1186/1471-2105-7-S5-S17
Title: Modelling study of dimerization in mammalian defensins
Authors: Suresh, A
Verma, C 
Keywords: Anionic phospholipids
Antimicrobial peptide
Bacterial membranes
Modelling studies
Non-specific binding
Physicochemical characteristics
Structural information
Therapeutic benefits
Amphipathicity
Defensins
Innate immunity
Mammalian species
Structural models
Dimerization
Monomers
Oligomers
Phospholipids
Bioinformatics
Model structures
Mammals
beta defensin 2
defensin
monomer
oligomer
beta defensin
cation
DEFB4 protein, human
defensin
unclassified drug
amino terminal sequence
article
carboxy terminal sequence
controlled study
dimerization
electricity
goat
human
mammal
molecular dynamics
mouse
nonhuman
physical chemistry
protein function
protein interaction
protein structure
sequence homology
sheep
animal
cell membrane
chemical structure
chemistry
computer simulation
genetics
metabolism
protein quaternary structure
sequence alignment
site directed mutagenesis
Bacteria (microorganisms)
Capra hircus
Mammalia
Ovis aries
Animals
beta-Defensins
Cations
Cell Membrane
Computer Simulation
Defensins
Dimerization
Humans
Mammals
Models, Molecular
Mutagenesis, Site-Directed
Protein Structure, Quaternary
Sequence Alignment
Issue Date: 2006
Citation: Suresh, A, Verma, C (2006). Modelling study of dimerization in mammalian defensins. BMC Bioinformatics 7 (SUPPL.5) : S17. ScholarBank@NUS Repository. https://doi.org/10.1186/1471-2105-7-S5-S17
Rights: Attribution 4.0 International
Abstract: Background: Defensins are antimicrobial peptides of innate immunity functioning by non-specific binding to anionic phospholipids in bacterial membranes. Their cationicity, amphipathicity and ability to oligomerize are considered key factors for their action. Based on structural information on human ?-defensin 2, we examine homologous defensins from various mammalian species for conserved functional physico-chemical characteristics. Results: Based on homology greater than 40%, structural models of 8 homologs of HBD-2 were constructed. A conserved pattern of electrostatics and dynamics was observed across 6 of the examined defensins; models backed by energetics suggest that the defensins in these 6 organisms are characterized by dimerization-linked enhanced functional potentials. In contrast, dimerization is not energetically favoured in the sheep, goat and mouse defensins, suggesting that they function efficiently as monomers. Conclusion: ?-defensin 2 from some mammals may work as monomers while those in others, including humans, work as oligomers. This could potentially be used to design human defensins that may be effective at lower concentrations and hence have therapeutic benefits.
Source Title: BMC Bioinformatics
URI: https://scholarbank.nus.edu.sg/handle/10635/178008
ISSN: 14712105
DOI: 10.1186/1471-2105-7-S5-S17
Rights: Attribution 4.0 International
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