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Bagher Seyedalipour

Bagher Seyedalipour

Academic rank: Associate Professor
ORCID: http://orcid.org/0000-0002-3854-9328
Education: PhD.
ScopusId: https://www.scopus.com/authid/detail.uri?authorId=56725735600
HIndex: 0/00
Faculty: Science
Address: Department of Cellular and Molecular, Faculty of Basic Sciences, University of Mazandaran, Babolsar, Iran
Phone: 01135302405

Research

Title
Role of charged residues of the “electrostatic loop” of hSOD1 in promotion of aggregation: Implications for the mechanism of ALS-associated mutations under amyloidogenic conditions
Type
JournalPaper
Keywords
Amyotrophic lateral sclerosis (ALS) Amyloidogenic conditions Human superoxide dismutase (hSOD1) G138E and T137R variants Molecular dynamics (MD) simulations
Year
2023
Journal International Journal of Biological Macromolecules
DOI
Researchers Elaheh Mavadat ، Bagher Seyedalipour ، Saman Hosseinkhani ، Abasalt Hosseinzadeh Colagar

Abstract

Protein misfolding and amyloid formation are hallmarks of numerous diseases, including amyotrophic lateral sclerosis (ALS), in which hSOD1 aggregation is involved in pathogenesis. We used two point mutations in the electrostatic loop, G138E and T137R, to analyze charge distribution under destabilizing circumstances to gain more about how ALS-linked mutations affect SOD1 protein stability or net repulsive charge. We show that protein charge is important in the ALS disease process using bioinformatics and experiments. The MD simulation findings demonstrate that the mutant protein differs significantly from WT SOD1, which is consistent with the experimental evidence. The specific activity of the wild type was 1.61 and 1.48 times higher than that of the G138E and T137R mutants, respectively. Under amyloid induction conditions, the intensity of intrinsic and ANS fluorescence in both mutants reduced. Increasing the content of β-sheet structures in mutants can be attributed to aggregation propensity, which was confirmed using CD polarimetry and FTIR spectroscopy. Our findings show that two ALS-related mutations promote the formation of amyloid-like aggregates at near physiological pH under destabilizing conditions, which were detected using spectroscopic probes such as Congo red and ThT fluorescence, and also further confirmation of amyloid-like species by TEM. Overall, our results provide evidence supporting the notion that negative charge changes combined with other destabilizing factors play an important role in increasing protein aggregation by reducing repulsive negative charges.