Computational screening of damaging nsSNPs in human SOD1 genes associated with amyotrophic lateral sclerosis identifies destabilising effects of G38R and G42D mutations through in silico evaluation

Samiksha Bhor; Sadia Haque Tonny; Susha Dinesh; Sameer Sharma

doi:10.1007/s40203-024-00191-7

Computational screening of damaging nsSNPs in human SOD1 genes associated with amyotrophic lateral sclerosis identifies destabilising effects of G38R and G42D mutations through in silico evaluation

In Silico Pharmacol. 2024 Mar 27;12(1):20. doi: 10.1007/s40203-024-00191-7. eCollection 2024.

Authors

Samiksha Bhor¹, Sadia Haque Tonny², Susha Dinesh¹, Sameer Sharma¹

Affiliations

¹ Department of Bioinformatics, BioNome, Bengaluru, Karnataka 560043 India.
² Department of Plant Pathology, Faculty of Agriculture, Bangladesh Agricultural University, Mymensingh, 2202 Bangladesh.

PMID: 38559706
PMCID: PMC10973320 (available on 2025-03-27)
DOI: 10.1007/s40203-024-00191-7

Abstract

Amyotrophic lateral sclerosis (ALS), a complicated neurodegenerative disorder affected by hereditary and environmental variables, is a condition. In this study, the genetic makeup of ALS is investigated, with a focus on the SOD1 gene's single-nucleotide polymorphisms (SNPs) and their ability to affect disease risk. Eleven high-risk missense variations that may impair the functionality of the SOD1 protein were discovered after a thorough examination of SNPs in the SOD1 gene. These mutations were chosen using a variety of prediction approaches, highlighting their importance in the aetiology of ALS. Notably, it was discovered that the stability of the SOD1 wild-type protein structure was compromised by the G38R and G42D SOD1 variants. Additionally, Edaravone, a possible ALS medication, showed a greater affinity for binding mutant SOD1 structures, pointing to potential personalised treatment possibilities. The high-risk SNPs discovered in this investigation seem to have functional effects, especially on the stability of proteins and their interactions with other molecules. This study clarifies the complex genetics of ALS and offers insights into how these genetic variations may affect the effectiveness of therapeutic interventions, particularly in the context of edaravone. In this study advances our knowledge of the genetic mechanisms causing ALS vulnerability and prospective therapeutic strategies. Future studies are necessary to confirm these results and close the gap between individualised clinical applications and improved ALS care.

Keywords: ALS; Edaravone; Genetic factor; Interaction; Missense mutation; SNP; SOD1 protein.

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