Md Jahirul Islam, Md Siddik Alom, Md Shahadat Hossain, Md Ackas Ali, Shaila Akter, Shafiqul Islam, M Obayed Ullah, Mohammad A Halim
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引用次数: 0
Abstract
ORF3a is a conserved accessory protein of SARS-CoV-2, linked to viral infection and pathogenesis, with acquired mutations at various locations. Previous studies have shown that the occurrence of the Q57H mutation is higher in comparison to other positions in ORF3a. This mutation is known to induce conformational changes, yet the extent of structural alteration and its role in the viral adaptation process remain unknown. Here we performed molecular dynamics (MD) simulations of wt-ORF3a, Q57H, and Q57A mutants to analyze structural changes caused by mutations compared to the native protein. The MD analysis revealed that Q57H and Q57A mutants show significant structural changes in the dimer conformation than the wt-ORF3a. This dimer conformer narrows down the ion channel cavity, which reduces Na + or K + permeability leading to decrease the antigenic response that can help the virus to escape the host immune system. Non-bonding interaction analysis shows the Q57H mutant has more interacting residues, resulting in more stability within dimer conformation than the wt-ORF3a and Q57A. Moreover, both mutant dimers (Q57H and Q57A) form a novel salt-bridge interaction at the same position between A:Asp142 and B:Lys61, whereas such an interaction is absent in the wt-ORF3a dimer. We have also noticed that the TM3 domain's flexibility in Q57H is increased because of strong inter-domain interactions of TM1 and TM2 within the dimer conformation. These unusual interactions and flexibility of Q57H mutant can have significant impacts on the SARS-CoV-2 adaptations, virulence, transmission, and immune system evasion. Our findings are consistent with the previous experimental data and provided details information on the structural perturbation in ORF3a caused by mutations, which can help better understand the structural change at the molecular level as well as the reason for the high virulence properties of this variant.Communicated by Ramaswamy H. Sarma.
ORF3a是SARS-CoV-2的一种保守的辅助蛋白,与病毒感染和发病机制有关,并在不同位置发生获得性突变。先前的研究表明,与ORF3a的其他位置相比,Q57H突变的发生率更高。已知这种突变可诱导构象变化,但结构改变的程度及其在病毒适应过程中的作用尚不清楚。在这里,我们对wt-ORF3a、Q57H和Q57A突变体进行了分子动力学(MD)模拟,以分析与天然蛋白相比,突变引起的结构变化。MD分析显示,与wt-ORF3a相比,Q57H和Q57A突变体的二聚体构象发生了显著的结构变化。这种二聚体构象缩小了离子通道腔,从而降低了Na +或K +的渗透性,从而减少了抗原反应,从而帮助病毒逃离宿主免疫系统。非键相互作用分析表明,与wt-ORF3a和Q57A相比,Q57H突变体具有更多的相互作用残基,在二聚体构象内具有更高的稳定性。此外,两种突变二聚体(Q57H和Q57A)在a:Asp142和B:Lys61之间的相同位置形成了一种新的盐桥相互作用,而wt-ORF3a二聚体中没有这种相互作用。我们还注意到,TM3结构域的灵活性在Q57H中增加,因为TM1和TM2在二聚体构象中具有很强的结构域间相互作用。Q57H突变体的这些不寻常的相互作用和灵活性可能对SARS-CoV-2的适应性、毒力、传播和免疫系统逃避产生重大影响。我们的发现与之前的实验数据一致,提供了突变引起ORF3a结构扰动的详细信息,有助于更好地了解该变异在分子水平上的结构变化以及该变异具有高毒力特性的原因。由Ramaswamy H. Sarma传达。
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