Computer-aided drug discovery of natural antiviral metabolites as potential SARS-CoV-2 helicase inhibitors

IF 1 4区 化学 Q4 CHEMISTRY, MULTIDISCIPLINARY
E. Elkaeed, I. Eissa, Abdulrahman M. Saleh, B. A. Alsfouk, A. Metwaly
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引用次数: 0

Abstract

In our quest to discover effective inhibitors against severe acute respiratory syndrome coronavirus 2 helicase, a diverse set of more than 300 naturally occurring antiviral metabolites was investigated. Employing advanced computational techniques, we initiated the selection process by analyzing and comparing the co-crystallized ligand (VXG) of the severe acute respiratory syndrome coronavirus 2 helicase protein (PDB ID: 5RMM) to identify compounds with structurally similar features and potential for comparable binding. Through structural similarity and pharmacophore research, 13 compounds that shared important characteristics with VXG were pinpointed. Subsequently, these candidates were subjected to molecular docking to identify seven compounds that demonstrated favorable energy profiles and accurate binding to the severe acute respiratory syndrome coronavirus 2 helicase. Among these, mycophenolic acid emerged as the most promising candidate. To ensure the safety and viability of the selected compounds, we conducted ADMET tests, which confirmed the favorable characteristics of mycophenolic acid, and the safety of atropine and plumbagin. Building on these results, we performed additional analyses on mycophenolic acid, including various molecular dynamics simulations. These investigations demonstrated that mycophenolic acid exhibited optimal binding to the severe acute respiratory syndrome coronavirus 2 helicase, maintaining flawless dynamics throughout the simulations. Furthermore, the Molecular Mechanics Poisson–Boltzmann Surface Area tests provided strong evidence that mycophenolic acid successfully formed a stable connection with the severe acute respiratory syndrome coronavirus 2 helicase, with a calculated free energy value of −294 kJ mol−1. These encouraging findings provide a solid foundation for further research, including in vitro and in vivo studies, on the three identified compounds. The potential efficacy of these compounds as treatment options for coronavirus-19 warrants further exploration and may hold significant promise in the ongoing fight against the pandemic.
计算机辅助药物发现天然抗病毒代谢物作为潜在的 SARS-CoV-2 螺旋酶抑制剂
为了发现对严重急性呼吸系统综合征冠状病毒 2 螺旋酶有效的抑制剂,我们研究了 300 多种天然存在的抗病毒代谢物。我们采用先进的计算技术,通过分析和比较严重急性呼吸道综合征冠状病毒 2 螺旋酶蛋白的共晶体配体(VXG)(PDB ID:5RMM),开始了筛选过程,以确定具有结构相似特征和潜在可比结合力的化合物。通过结构相似性和药理研究,确定了 13 种与 VXG 具有相同重要特征的化合物。随后,对这些候选化合物进行了分子对接,最终确定了 7 种化合物,这些化合物显示出良好的能量曲线,并能与严重急性呼吸系统综合征冠状病毒 2 螺旋酶准确结合。其中,霉酚酸成为最有希望的候选化合物。为了确保所选化合物的安全性和可行性,我们进行了 ADMET 试验,结果证实了霉酚酸的有利特性,以及阿托品和普鲁巴金的安全性。在这些结果的基础上,我们对霉酚酸进行了更多分析,包括各种分子动力学模拟。这些研究表明,霉酚酸与严重急性呼吸系统综合征冠状病毒 2 螺旋酶的结合效果最佳,在整个模拟过程中都保持了完美的动态特性。此外,分子力学泊松-玻尔兹曼表面积测试提供了有力证据,证明霉酚酸成功地与严重急性呼吸系统综合征冠状病毒 2 螺旋酶形成了稳定的连接,计算出的自由能值为 -294 kJ mol-1。这些令人鼓舞的发现为进一步研究(包括体外和体内研究)这三种已发现的化合物奠定了坚实的基础。这些化合物作为冠状病毒-19 治疗方案的潜在疗效值得进一步探索,并可能在当前抗击大流行病的斗争中大有可为。
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来源期刊
Journal of Chemical Research
Journal of Chemical Research CHEMISTRY, MULTIDISCIPLINARY-
CiteScore
2.30
自引率
0.00%
发文量
66
审稿时长
1.0 months
期刊介绍: The Journal of Chemical Research is a monthly journal which has a broad international authorship and publishes research papers and reviews in all branches of experimental chemistry. Established in 1977 as a joint venture by the British, French and German chemical societies it maintains the high standards set by the founding societies. Each paper is independently peer reviewed and only carefully evaluated contributions are accepted. Recent papers have described new synthetic methods, new heterocyclic compounds, new natural products, and the inorganic chemistry of metal complexes.
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