Beta-strand interfaces of non-dimeric protein oligomers are characterized by scattered charged residue patterns.

Beta-strand interfaces of non-dimeric protein oligomers are characterized by scattered charged residue patterns.

Protein oligomers are formed either permanently, transiently or even by default. The protein chains are associated through intermolecular interactions constituting the protein interface. The protein interfaces of 40 soluble protein oligomers of stœchiometries above two are investigated using a quant...

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Main Authors: Giovanni Feverati, Mounia Achoch, Jihad Zrimi, Laurent Vuillon, Claire Lesieur
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3322119?pdf=render
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spelling doaj-5ce0c4147147448abfd0936f7037db8a2020-11-25T00:02:41ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0174e3255810.1371/journal.pone.0032558Beta-strand interfaces of non-dimeric protein oligomers are characterized by scattered charged residue patterns.Giovanni FeveratiMounia AchochJihad ZrimiLaurent VuillonClaire LesieurProtein oligomers are formed either permanently, transiently or even by default. The protein chains are associated through intermolecular interactions constituting the protein interface. The protein interfaces of 40 soluble protein oligomers of stœchiometries above two are investigated using a quantitative and qualitative methodology, which analyzes the x-ray structures of the protein oligomers and considers their interfaces as interaction networks. The protein oligomers of the dataset share the same geometry of interface, made by the association of two individual β-strands (β-interfaces), but are otherwise unrelated. The results show that the β-interfaces are made of two interdigitated interaction networks. One of them involves interactions between main chain atoms (backbone network) while the other involves interactions between side chain and backbone atoms or between only side chain atoms (side chain network). Each one has its own characteristics which can be associated to a distinct role. The secondary structure of the β-interfaces is implemented through the backbone networks which are enriched with the hydrophobic amino acids favored in intramolecular β-sheets (MCWIV). The intermolecular specificity is provided by the side chain networks via positioning different types of charged residues at the extremities (arginine) and in the middle (glutamic acid and histidine) of the interface. Such charge distribution helps discriminating between sequences of intermolecular β-strands, of intramolecular β-strands and of β-strands forming β-amyloid fibers. This might open new venues for drug designs and predictive tool developments. Moreover, the β-strands of the cholera toxin B subunit interface, when produced individually as synthetic peptides, are capable of inhibiting the assembly of the toxin into pentamers. Thus, their sequences contain the features necessary for a β-interface formation. Such β-strands could be considered as 'assemblons', independent associating units, by homology to the foldons (independent folding unit). Such property would be extremely valuable in term of assembly inhibitory drug development.http://europepmc.org/articles/PMC3322119?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Giovanni Feverati
Mounia Achoch
Jihad Zrimi
Laurent Vuillon
Claire Lesieur
spellingShingle Giovanni Feverati
Mounia Achoch
Jihad Zrimi
Laurent Vuillon
Claire Lesieur
Beta-strand interfaces of non-dimeric protein oligomers are characterized by scattered charged residue patterns.
PLoS ONE
author_facet Giovanni Feverati
Mounia Achoch
Jihad Zrimi
Laurent Vuillon
Claire Lesieur
author_sort Giovanni Feverati
title Beta-strand interfaces of non-dimeric protein oligomers are characterized by scattered charged residue patterns.
title_short Beta-strand interfaces of non-dimeric protein oligomers are characterized by scattered charged residue patterns.
title_full Beta-strand interfaces of non-dimeric protein oligomers are characterized by scattered charged residue patterns.
title_fullStr Beta-strand interfaces of non-dimeric protein oligomers are characterized by scattered charged residue patterns.
title_full_unstemmed Beta-strand interfaces of non-dimeric protein oligomers are characterized by scattered charged residue patterns.
title_sort beta-strand interfaces of non-dimeric protein oligomers are characterized by scattered charged residue patterns.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Protein oligomers are formed either permanently, transiently or even by default. The protein chains are associated through intermolecular interactions constituting the protein interface. The protein interfaces of 40 soluble protein oligomers of stœchiometries above two are investigated using a quantitative and qualitative methodology, which analyzes the x-ray structures of the protein oligomers and considers their interfaces as interaction networks. The protein oligomers of the dataset share the same geometry of interface, made by the association of two individual β-strands (β-interfaces), but are otherwise unrelated. The results show that the β-interfaces are made of two interdigitated interaction networks. One of them involves interactions between main chain atoms (backbone network) while the other involves interactions between side chain and backbone atoms or between only side chain atoms (side chain network). Each one has its own characteristics which can be associated to a distinct role. The secondary structure of the β-interfaces is implemented through the backbone networks which are enriched with the hydrophobic amino acids favored in intramolecular β-sheets (MCWIV). The intermolecular specificity is provided by the side chain networks via positioning different types of charged residues at the extremities (arginine) and in the middle (glutamic acid and histidine) of the interface. Such charge distribution helps discriminating between sequences of intermolecular β-strands, of intramolecular β-strands and of β-strands forming β-amyloid fibers. This might open new venues for drug designs and predictive tool developments. Moreover, the β-strands of the cholera toxin B subunit interface, when produced individually as synthetic peptides, are capable of inhibiting the assembly of the toxin into pentamers. Thus, their sequences contain the features necessary for a β-interface formation. Such β-strands could be considered as 'assemblons', independent associating units, by homology to the foldons (independent folding unit). Such property would be extremely valuable in term of assembly inhibitory drug development.
url http://europepmc.org/articles/PMC3322119?pdf=render
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