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Iran J Biotechnol. 2022 Oct 1;20(4):e3178. doi: 10.30498/ijb.2022.310249.3178. eCollection 2022 Oct.
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PSP-GNM: Predicting Protein Stability Changes upon Point Mutations with a Gaussian Network Model.PSP-GNM:基于高斯网络模型预测点突变对蛋白质稳定性的影响。
Int J Mol Sci. 2022 Sep 14;23(18):10711. doi: 10.3390/ijms231810711.
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SOD1 gains pro-oxidant activity upon aberrant oligomerization: change in enzymatic activity by intramolecular disulfide bond cleavage.SOD1 在异常寡聚化后获得促氧化剂活性:通过分子内二硫键断裂改变酶活性。
Sci Rep. 2022 Jul 11;12(1):11750. doi: 10.1038/s41598-022-15701-w.
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Zinc binding loop mutations of hSOD1 promote amyloid fibrils under physiological conditions: Implications for initiation of amyotrophic lateral sclerosis.锌结合环突变的 hSOD1 在生理条件下促进淀粉样纤维形成:肌萎缩侧索硬化症发病机制的研究。
Biochimie. 2022 Aug;199:170-181. doi: 10.1016/j.biochi.2022.05.001. Epub 2022 May 7.
5
Conformational dynamics of superoxide dismutase (SOD1) in osmolytes: a molecular dynamics simulation study.超氧化物歧化酶(SOD1)在渗透剂中的构象动力学:分子动力学模拟研究
RSC Adv. 2020 Jul 30;10(46):27598-27614. doi: 10.1039/d0ra02151b. eCollection 2020 Jul 21.
6
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SOD1 mutations associated with amyotrophic lateral sclerosis analysis of variant severity.与肌萎缩侧索硬化症相关的 SOD1 突变分析:变异严重程度。
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SAAFEC-SEQ: A Sequence-Based Method for Predicting the Effect of Single Point Mutations on Protein Thermodynamic Stability.SAAFEC-SEQ:一种基于序列的方法,用于预测单点突变对蛋白质热力学稳定性的影响。
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Clinical and Molecular Landscape of ALS Patients with Mutations: Novel Pathogenic Variants and Novel Phenotypes. A Single ALS Center Study.ALS 患者突变的临床和分子特征:新的致病性变异和新的表型。一项单 ALS 中心研究。
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肌萎缩侧索硬化症相关的人超氧化物歧化酶1(hSOD1)在脱辅基/结合辅基状态下二聚体界面残基的计算机模拟分析及分子动力学模拟的计算洞察:实验与生物信息学相结合的视角

Computational insight into in silico analysis and molecular dynamics simulation of the dimer interface residues of ALS-linked hSOD1 forms in apo/holo states: a combined experimental and bioinformatic perspective.

作者信息

Zaji Hamza Dakhil, Seyedalipour Bagher, Hanun Haider Munzer, Baziyar Payam, Hosseinkhani Saman, Akhlaghi Mona

机构信息

Department of Molecular and Cell Biology, Faculty of Basic Science, University of Mazandaran, Babolsar, Iran.

Department of Biochemistry, Faculty of Biological Sciences, Tarbiat Modares University, Tehran, Iran.

出版信息

3 Biotech. 2023 Mar;13(3):92. doi: 10.1007/s13205-023-03514-1. Epub 2023 Feb 21.

DOI:10.1007/s13205-023-03514-1
PMID:36845075
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9944573/
Abstract

The aggregation of misfolded SOD1 proteins in neurodegenerative illnesses is a key pathological hallmark in amyotrophic lateral sclerosis (ALS). SOD1 is stabilized and enzymatically activated after binding to Cu/Zn and forming intramolecular disulfide. SOD1 aggregation/oligomerization is triggered by the dissociation of Cu and/or Zn ions. Therefore, we compared the possible effects of ALS-associated point mutations of the holo/apo forms of WT/I149T/V148G SOD1 variants located at the dimer interface to determine structural characterization using spectroscopic methods, computational approaches as well as molecular dynamics (MD) simulations. Predictive results of computational analysis of single-nucleotide polymorphisms (SNPs) suggested that mutant SOD1 has a deleterious effect on activity and structure destabilization. MD data analysis indicated that changes in flexibility, stability, hydrophobicity of the protein as well as increased intramolecular interactions of apo-SOD1 were more than holo-SOD1. Furthermore, a decrease in enzymatic activity in apo-SOD1 was observed compared to holo-SOD1. Comparative intrinsic and ANS fluorescence results of holo/apo-WT-hSOD1 and mutants indicated structural alterations in the local environment of tryptophan residue and hydrophobic patches, respectively. Experimental and MD data supported that substitution effect and metal deficiency of mutants (apo forms) in the dimer interface may promote the tendency to protein mis-folding and aggregation, consequently disrupting the dimer-monomer equilibrium and increased propensity to dissociation dimer into SOD-monomer ultimately leading to loss of stability and function. Overall, data analysis of apo/holo SOD1 forms on protein structure and function using computational and experimental studies will contribute to a better understanding of ALS pathogenicity.

摘要

在神经退行性疾病中,错误折叠的超氧化物歧化酶1(SOD1)蛋白聚集是肌萎缩侧索硬化症(ALS)的一个关键病理标志。SOD1与铜/锌结合并形成分子内二硫键后会稳定下来并被酶激活。SOD1的聚集/寡聚化是由铜和/或锌离子的解离引发的。因此,我们比较了位于二聚体界面的野生型/ I149T / V148G SOD1变体的全酶/脱辅基形式的ALS相关点突变的可能影响,以使用光谱方法、计算方法以及分子动力学(MD)模拟来确定结构特征。单核苷酸多态性(SNP)的计算分析预测结果表明,突变型SOD1对活性和结构不稳定有有害影响。MD数据分析表明,脱辅基SOD1在蛋白质的柔韧性、稳定性、疏水性以及分子内相互作用增加方面的变化比全酶SOD1更大。此外,与全酶SOD1相比,观察到脱辅基SOD1的酶活性降低。全酶/脱辅基野生型人SOD1和突变体的比较固有荧光和ANS荧光结果分别表明色氨酸残基局部环境和疏水区域的结构改变。实验和MD数据支持二聚体界面处突变体(脱辅基形式)的取代效应和金属缺乏可能会促进蛋白质错误折叠和聚集的倾向,从而破坏二聚体 - 单体平衡,并增加二聚体解离为SOD单体的倾向,最终导致稳定性和功能丧失。总体而言,使用计算和实验研究对脱辅基/全酶SOD1形式的蛋白质结构和功能进行数据分析将有助于更好地理解ALS的致病性。