ALS-causing mutations in profilin-1 alter its conformational dynamics: A computational approach to explain propensity for aggregation

Profilin-1 (PFN1) is a 140-amino-acid protein with two distinct binding sites―one for actin and one for poly-L-proline (PLP). The best-described function of PFN1 is to catalyze actin elongation and polymerization. Thus far, eight DNA mutations in the PFN1 gene encoding the PFN1 protein are associate...

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Autores principales: Kiaei, Mahmoud, Balasubramaniam, Meenakshisundaram, Govind Kumar, Vivek, Shmookler Reis, Robert J., Moradi, Mahmoud, Varughese, Kottayil I.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2018
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6117255/
https://www.ncbi.nlm.nih.gov/pubmed/30166578
http://dx.doi.org/10.1038/s41598-018-31199-7
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author Kiaei, Mahmoud
Balasubramaniam, Meenakshisundaram
Govind Kumar, Vivek
Shmookler Reis, Robert J.
Moradi, Mahmoud
Varughese, Kottayil I.
author_facet Kiaei, Mahmoud
Balasubramaniam, Meenakshisundaram
Govind Kumar, Vivek
Shmookler Reis, Robert J.
Moradi, Mahmoud
Varughese, Kottayil I.
author_sort Kiaei, Mahmoud
collection PubMed
description Profilin-1 (PFN1) is a 140-amino-acid protein with two distinct binding sites―one for actin and one for poly-L-proline (PLP). The best-described function of PFN1 is to catalyze actin elongation and polymerization. Thus far, eight DNA mutations in the PFN1 gene encoding the PFN1 protein are associated with human amyotrophic lateral sclerosis (ALS). We and others recently showed that two of these mutations (Gly118Val or G118V and Cys71Gly or C71G) cause ALS in rodents. In vitro studies suggested that Met114Thr and Thr109Met cause the protein to behave abnormally and cause neurotoxicity. The mechanism by which a single amino acid change in human PFN1 causes the degeneration of motor neurons is not known. In this study, we investigated the structural perturbations of PFN1 caused by each ALS-associated mutation. We used molecular dynamics simulations to assess how these mutations alter the secondary and tertiary structures of human PFN1. Herein, we present our in silico data and analysis on the effect of G118V and T109M mutations on PFN1 and its interactions with actin and PLP. The substitution of valine for glycine reduces the conformational flexibility of the loop region between the α-helix and β-strand and enhances the hydrophobicity of the region. Our in silico analysis of T109M indicates that this mutation alters the shape of the PLP-binding site and reduces the flexibility of this site. Simulation studies of PFN1 in its wild type (WT) and mutant forms (both G118V and T109M mutants) revealed differential fluctuation patterns and the formation of salt bridges and hydrogen bonds between critical residues that may shed light on differences between WT and mutant PFN1. In particular, we hypothesize that the flexibility of the actin- and PLP-binding sites in WT PFN1 may allow the protein to adopt slightly different conformations in its free and bound forms. These findings provide new insights into how each of these mutations in PFN1 might increase its propensity for misfolding and aggregation, leading to its dysfunction.
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spelling pubmed-61172552018-09-05 ALS-causing mutations in profilin-1 alter its conformational dynamics: A computational approach to explain propensity for aggregation Kiaei, Mahmoud Balasubramaniam, Meenakshisundaram Govind Kumar, Vivek Shmookler Reis, Robert J. Moradi, Mahmoud Varughese, Kottayil I. Sci Rep Article Profilin-1 (PFN1) is a 140-amino-acid protein with two distinct binding sites―one for actin and one for poly-L-proline (PLP). The best-described function of PFN1 is to catalyze actin elongation and polymerization. Thus far, eight DNA mutations in the PFN1 gene encoding the PFN1 protein are associated with human amyotrophic lateral sclerosis (ALS). We and others recently showed that two of these mutations (Gly118Val or G118V and Cys71Gly or C71G) cause ALS in rodents. In vitro studies suggested that Met114Thr and Thr109Met cause the protein to behave abnormally and cause neurotoxicity. The mechanism by which a single amino acid change in human PFN1 causes the degeneration of motor neurons is not known. In this study, we investigated the structural perturbations of PFN1 caused by each ALS-associated mutation. We used molecular dynamics simulations to assess how these mutations alter the secondary and tertiary structures of human PFN1. Herein, we present our in silico data and analysis on the effect of G118V and T109M mutations on PFN1 and its interactions with actin and PLP. The substitution of valine for glycine reduces the conformational flexibility of the loop region between the α-helix and β-strand and enhances the hydrophobicity of the region. Our in silico analysis of T109M indicates that this mutation alters the shape of the PLP-binding site and reduces the flexibility of this site. Simulation studies of PFN1 in its wild type (WT) and mutant forms (both G118V and T109M mutants) revealed differential fluctuation patterns and the formation of salt bridges and hydrogen bonds between critical residues that may shed light on differences between WT and mutant PFN1. In particular, we hypothesize that the flexibility of the actin- and PLP-binding sites in WT PFN1 may allow the protein to adopt slightly different conformations in its free and bound forms. These findings provide new insights into how each of these mutations in PFN1 might increase its propensity for misfolding and aggregation, leading to its dysfunction. Nature Publishing Group UK 2018-08-30 /pmc/articles/PMC6117255/ /pubmed/30166578 http://dx.doi.org/10.1038/s41598-018-31199-7 Text en © The Author(s) 2018 Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/.
spellingShingle Article
Kiaei, Mahmoud
Balasubramaniam, Meenakshisundaram
Govind Kumar, Vivek
Shmookler Reis, Robert J.
Moradi, Mahmoud
Varughese, Kottayil I.
ALS-causing mutations in profilin-1 alter its conformational dynamics: A computational approach to explain propensity for aggregation
title ALS-causing mutations in profilin-1 alter its conformational dynamics: A computational approach to explain propensity for aggregation
title_full ALS-causing mutations in profilin-1 alter its conformational dynamics: A computational approach to explain propensity for aggregation
title_fullStr ALS-causing mutations in profilin-1 alter its conformational dynamics: A computational approach to explain propensity for aggregation
title_full_unstemmed ALS-causing mutations in profilin-1 alter its conformational dynamics: A computational approach to explain propensity for aggregation
title_short ALS-causing mutations in profilin-1 alter its conformational dynamics: A computational approach to explain propensity for aggregation
title_sort als-causing mutations in profilin-1 alter its conformational dynamics: a computational approach to explain propensity for aggregation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6117255/
https://www.ncbi.nlm.nih.gov/pubmed/30166578
http://dx.doi.org/10.1038/s41598-018-31199-7
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