Recognition of interaction interface residues in low-resolution structures of protein assemblies solely from the positions of C(alpha) atoms.

BACKGROUND: The number of available structures of large multi-protein assemblies is quite small. Such structures provide phenomenal insights on the organization, mechanism of formation and functional properties of the assembly. Hence detailed analysis of such structures is highly rewarding. However,...

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Main Authors: Rupali A Gadkari, Deepthi Varughese, N Srinivasan
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2009-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC2641018?pdf=render
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spelling doaj-7611bbfc528244e7ad4fe7bc21acac092020-11-24T21:55:55ZengPublic Library of Science (PLoS)PLoS ONE1932-62032009-01-0142e447610.1371/journal.pone.0004476Recognition of interaction interface residues in low-resolution structures of protein assemblies solely from the positions of C(alpha) atoms.Rupali A GadkariDeepthi VarugheseN SrinivasanBACKGROUND: The number of available structures of large multi-protein assemblies is quite small. Such structures provide phenomenal insights on the organization, mechanism of formation and functional properties of the assembly. Hence detailed analysis of such structures is highly rewarding. However, the common problem in such analyses is the low resolution of these structures. In the recent times a number of attempts that combine low resolution cryo-EM data with higher resolution structures determined using X-ray analysis or NMR or generated using comparative modeling have been reported. Even in such attempts the best result one arrives at is the very course idea about the assembly structure in terms of trace of the C(alpha) atoms which are modeled with modest accuracy. METHODOLOGY/PRINCIPAL FINDINGS: In this paper first we present an objective approach to identify potentially solvent exposed and buried residues solely from the position of C(alpha) atoms and amino acid sequence using residue type-dependent thresholds for accessible surface areas of C(alpha). We extend the method further to recognize potential protein-protein interface residues. CONCLUSION/ SIGNIFICANCE: Our approach to identify buried and exposed residues solely from the positions of C(alpha) atoms resulted in an accuracy of 84%, sensitivity of 83-89% and specificity of 67-94% while recognition of interfacial residues corresponded to an accuracy of 94%, sensitivity of 70-96% and specificity of 58-94%. Interestingly, detailed analysis of cases of mismatch between recognition of interface residues from C(alpha) positions and all-atom models suggested that, recognition of interfacial residues using C(alpha) atoms only correspond better with intuitive notion of what is an interfacial residue. Our method should be useful in the objective analysis of structures of protein assemblies when positions of only (alpha) positions are available as, for example, in the cases of integration of cryo-EM data and high resolution structures of the components of the assembly.http://europepmc.org/articles/PMC2641018?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Rupali A Gadkari
Deepthi Varughese
N Srinivasan
spellingShingle Rupali A Gadkari
Deepthi Varughese
N Srinivasan
Recognition of interaction interface residues in low-resolution structures of protein assemblies solely from the positions of C(alpha) atoms.
PLoS ONE
author_facet Rupali A Gadkari
Deepthi Varughese
N Srinivasan
author_sort Rupali A Gadkari
title Recognition of interaction interface residues in low-resolution structures of protein assemblies solely from the positions of C(alpha) atoms.
title_short Recognition of interaction interface residues in low-resolution structures of protein assemblies solely from the positions of C(alpha) atoms.
title_full Recognition of interaction interface residues in low-resolution structures of protein assemblies solely from the positions of C(alpha) atoms.
title_fullStr Recognition of interaction interface residues in low-resolution structures of protein assemblies solely from the positions of C(alpha) atoms.
title_full_unstemmed Recognition of interaction interface residues in low-resolution structures of protein assemblies solely from the positions of C(alpha) atoms.
title_sort recognition of interaction interface residues in low-resolution structures of protein assemblies solely from the positions of c(alpha) atoms.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2009-01-01
description BACKGROUND: The number of available structures of large multi-protein assemblies is quite small. Such structures provide phenomenal insights on the organization, mechanism of formation and functional properties of the assembly. Hence detailed analysis of such structures is highly rewarding. However, the common problem in such analyses is the low resolution of these structures. In the recent times a number of attempts that combine low resolution cryo-EM data with higher resolution structures determined using X-ray analysis or NMR or generated using comparative modeling have been reported. Even in such attempts the best result one arrives at is the very course idea about the assembly structure in terms of trace of the C(alpha) atoms which are modeled with modest accuracy. METHODOLOGY/PRINCIPAL FINDINGS: In this paper first we present an objective approach to identify potentially solvent exposed and buried residues solely from the position of C(alpha) atoms and amino acid sequence using residue type-dependent thresholds for accessible surface areas of C(alpha). We extend the method further to recognize potential protein-protein interface residues. CONCLUSION/ SIGNIFICANCE: Our approach to identify buried and exposed residues solely from the positions of C(alpha) atoms resulted in an accuracy of 84%, sensitivity of 83-89% and specificity of 67-94% while recognition of interfacial residues corresponded to an accuracy of 94%, sensitivity of 70-96% and specificity of 58-94%. Interestingly, detailed analysis of cases of mismatch between recognition of interface residues from C(alpha) positions and all-atom models suggested that, recognition of interfacial residues using C(alpha) atoms only correspond better with intuitive notion of what is an interfacial residue. Our method should be useful in the objective analysis of structures of protein assemblies when positions of only (alpha) positions are available as, for example, in the cases of integration of cryo-EM data and high resolution structures of the components of the assembly.
url http://europepmc.org/articles/PMC2641018?pdf=render
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