Comparative Structural Analysis of Human ACE2 Receptor with Spike Protein of SARS-CoV-2 Variants: Implications to Understand Infectivity of the Virus.

Q2 Biochemistry, Genetics and Molecular Biology

Advances and Applications in Bioinformatics and Chemistry Pub Date : 2022-06-16 eCollection Date: 2022-01-01 DOI:10.2147/AABC.S360787

Tirthankar Koley, Arunima Goswami, Manoj Kumar, Neelam Upadhyay, Gururao Hariprasad

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Abstract

Purpose: Spike protein on SARS-CoV-2 virus plays an integral part during infection as cell entry depends on binding of this protein to human ACE2 receptor. Understanding of infectivity by these variants necessitates a comparative structural analysis of complexes of spike protein-receptor binding domain (RBD) of these variants to receptor.

Methodology: Wild type SARS-CoV-2 spike protein sequence was retrieved from the UniProt database, and mutations of five variants at receptor binding domain were manually incorporated and aligned using Clustal Omega. Crystal structure complexes of human ACE2 receptor with spike protein RBD domain of SARS-CoV-2 variants of wild type, α, β, and δ were extracted from the RCSB database. Wild type SARS-CoV-2 complex with receptor was used as template to generate model complexes of receptor with spike protein RBD of γ and omicron variants through WinCoot program. These were energy minimized and validated and molecular dynamic simulation was performed using Desmond simulation program.

Results: Mutations are distributed across the entire length of RBD, but the maximum number of mutations are seen at 11 positions within binding interface motifs of six variant sequences. Interface of spike protein RBDs with human ACE2-receptor shows different mix of hydrogen bonded and ionic interactions. Alpha and β variants have few interactions, while γ and δ variants have higher number of interactions compared to wild type variant. Omicron variant, with 10 polar interactions including two ionic bonds, has the highest binding energy.

Conclusion: Different mutations on RBD of spike protein results in varying quantity and quality of interactions, thereby affecting potency of each variant. Variations in binding are due to interactions of mutant residues and induced conformational changes on loops of RBDs. Variants α and β have a low potency, while, γ, δ, and omicron have a higher potency. These results correlate with viral infectivity and place clinical observations in the right perspective.

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人类 ACE2 受体与 SARS-CoV-2 变体尖峰蛋白的结构比较分析：了解病毒传染性的意义

目的：SARS-CoV-2病毒上的尖峰蛋白在感染过程中起着不可或缺的作用，因为细胞的进入取决于该蛋白与人类ACE2受体的结合。要了解这些变体的感染性，就必须对这些变体的尖峰蛋白-受体结合域（RBD）与受体的复合物进行结构比较分析：方法：从UniProt数据库中检索野生型SARS-CoV-2尖峰蛋白序列，人工加入受体结合域的五个变体突变，并使用Clustal Omega进行比对。从 RCSB 数据库中提取了人类 ACE2 受体与 SARS-CoV-2 野生型、α、β 和 δ 变种的尖峰蛋白 RBD 结构域的晶体结构复合物。以野生型 SARS-CoV-2 与受体的复合物为模板，通过 WinCoot 程序生成受体与γ 和 omicron 变体的尖峰蛋白 RBD 的模型复合物。对这些模型进行了能量最小化和验证，并使用 Desmond 模拟程序进行了分子动力学模拟：结果：突变分布在 RBD 的整个长度上，但在六个变体序列的结合界面图案的 11 个位置上突变数量最多。尖峰蛋白 RBD 与人类 ACE2 受体的结合界面显示出不同的氢键和离子相互作用组合。与野生型变体相比，α 和 β 变体的相互作用较少，而 γ 和 δ 变体的相互作用较多。Omicron变体有10个极性相互作用，包括两个离子键，其结合能最高：结论：尖峰蛋白 RBD 上的不同突变会导致相互作用的数量和质量不同，从而影响每个变体的效力。结合力的变化是由于突变残基的相互作用和 RBD 环上的构象变化引起的。变体 α 和 β 的效力较低，而 γ、δ 和 omicron 的效力较高。这些结果与病毒的感染性相关，并使临床观察具有正确的视角。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Advances and Applications in Bioinformatics and Chemistry Biochemistry, Genetics and Molecular Biology-Biochemistry, Genetics and Molecular Biology (miscellaneous)

CiteScore

6.50

自引率

0.00%

发文量

审稿时长

16 weeks