离子强度对a - β1-42肽聚集倾向的影响:一项硅研究
引用次数: 0
摘要
应激条件下细胞内错误折叠蛋白的聚集可能导致几种神经退行性疾病。淀粉样蛋白- β (a - β1-42)肽是阿尔茨海默病的致病因子,在压力下有折叠成β片的倾向,形成聚集的淀粉样斑块。这受pH值、温度、金属离子、残基突变和溶液离子强度等因素的影响。有几项研究强调了离子强度在影响Aβ1-42肽的折叠和聚集倾向中的重要性。为了了解溶液离子强度对a - β1-42肽聚集倾向的影响,采用计算方法。在本研究中,将a - β1-42肽单体置于(i) 0 M、(ii) 0.15 M和(iii) 0.30 M浓度的NaCl溶液中进行分子动力学(MD)模拟。为了准备MD模拟的输入文件,我们使用了amberff99sb力场。利用CPPtraj工具分析了a - β1-42肽单体在溶液微分强度下的构象动力学。通过MD轨迹分析,我们发现随着溶液离子强度的增加,a - β1-42肽单体的聚集倾向减弱。从RMSD和SASA分析中,我们注意到a - β1-42肽单体的构象随着溶液离子强度的增加而快速变化。此外,从旋转半径(Rg)分析中,我们观察到Aβ1-42肽单体在中等离子强度的溶液中更加致密。β1-42肽也被发现在中等和较高的离子强度溶液中保持其螺旋二级结构。a - β1-42肽单体的扩散系数也随溶液离子强度的变化而变化。我们观察到,在中等离子强度的溶液中,a β1-42肽的扩散系数相对较高。我们的计算研究结果强调了溶液的离子强度对a - β1-42肽单体的构象动力学和聚集倾向的显著影响。本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effect of Ionic Strength on the Aggregation Propensity of Aβ1-42 Peptide: An In-silico Study
Aggregation of misfolded proteins under stress conditions in the cell
might lead to several neurodegenerative disorders. Amyloid-beta (Aβ1-42) peptide, the causative
agent of Alzheimer’s disease, has the propensity to fold into β-sheets under stress, forming
aggregated amyloid plaques. This is influenced by factors such as pH, temperature, metal
ions, mutation of residues, and ionic strength of the solution. There are several studies that
have highlighted the importance of ionic strength in affecting the folding and aggregation
propensity of Aβ1-42 peptide.
To understand the effect of ionic strength of the solution on the aggregation propensity
of Aβ1-42 peptide, using computational approaches.
In this study, Molecular Dynamics (MD) simulations were performed
on Aβ1-42 peptide monomer placed in (i) 0 M, (ii) 0.15 M, and (iii) 0.30 M concentration
of NaCl solution. To prepare the input files for the MD simulations, we have used the
Amberff99SB force field. The conformational dynamics of Aβ1-42 peptide monomer in different
ionic strengths of the solutions were illustrated from the analysis of the corresponding
MD trajectory using the CPPtraj tool.
From the MD trajectory analysis, we observe that with an increase in the ionic
strength of the solution, Aβ1-42 peptide monomer shows a lesser tendency to undergo aggregation.
From RMSD and SASA analysis, we noticed that Aβ1-42 peptide monomer undergoes
a rapid change in conformation with an increase in the ionic strength of the solution. In addition,
from the radius of gyration (Rg) analysis, we observed Aβ1-42 peptide monomer to be
more compact at moderate ionic strength of the solution. Aβ1-42 peptide was also found to
hold its helical secondary structure at moderate and higher ionic strengths of the solution.
The diffusion coefficient of Aβ1-42 peptide monomer was also found to vary with the ionic
strength of the solution. We observed a relatively higher diffusion coefficient value for Aβ1-42
peptide at moderate ionic strength of the solution.
Our findings from this computational study highlight the marked effect of ionic
strength of the solution on the conformational dynamics and aggregation propensity of Aβ1-42
peptide monomer.
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来源期刊
Current Chemical Biology
Medicine-Biochemistry (medical)
CiteScore
1.40
自引率
0.00%
发文量
16
期刊介绍:
Current Chemical Biology aims to publish full-length and mini reviews on exciting new developments at the chemistry-biology interface, covering topics relating to Chemical Synthesis, Science at Chemistry-Biology Interface and Chemical Mechanisms of Biological Systems. Current Chemical Biology covers the following areas: Chemical Synthesis (Syntheses of biologically important macromolecules including proteins, polypeptides, oligonucleotides, oligosaccharides etc.; Asymmetric synthesis; Combinatorial synthesis; Diversity-oriented synthesis; Template-directed synthesis; Biomimetic synthesis; Solid phase biomolecular synthesis; Synthesis of small biomolecules: amino acids, peptides, lipids, carbohydrates and nucleosides; and Natural product synthesis).
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