Boswellic acid derived molecules as SARS-CoV-2 spike protein inhibitors: A comprehensive virtual screening, triplicate molecular dynamic simulation and biochemical validation.

IF 3.5 4区医学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY

Current medicinal chemistry Pub Date : 2025-10-06 DOI:10.2174/0109298673354901250402143533

Atta Ullah, Muhammad Waqas, Saeed Ullah, Sobia Ahsan Halim, Satya Kumar Avula, Sadeeq Ur Rehman, Najeeb Ur Rehman, Magda H Abdellattif, Ajmal Khan, Ahmed Al-Harrasi

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引用次数: 0

Abstract

Background: Coronavirus disease (COVID-19) is a highly infective disease caused by SARS-CoV-2. The SARS-CoV-2 spike protein binds with the human ACE2 receptor to facilitate viral entry into the host cell; therefore, spike protein serves as a potential target for drug development.

Objective: Keeping in view the significance of SARS-CoV-2 spike protein for viral replications, in the current study, we identified the potent inhibitors against SARS-CoV-2 spike protein in order to combat the viral infection.

Methods: In the current study, we screened an in-house library of ~900 natural and synthesized compounds against the spike protein receptor binding domain (RBD) using a structure-based virtual approach, followed by an in-vitro inhibition bioassay.

Results: Seven (C1-C7) potent compounds were identified with docking scores ≥ -6.66 Kcal/mol; their drug-likeness, pharmacokinetic, and pharmacodynamic characteristics were excellent with no toxic effect. Those molecules were subjected to a triplicate simulation for 200 ns, which further confirmed their stable binding with RBD. This tight packing of complexes was reflected by calculated binding free energy, which disclosed higher binding free energy of C4, C7 and C6 than C1-C3, while predicted entropic energy demonstrates higher values for C4, C7 and C1 than the rest of the compounds, indicating more thermodynamic stability in protein due to conformational changes in spike protein induced by binding of C4, C7 and C1. These computational analyses were later validated through in-vitro bioassay. Remarkably, C2-C7 displayed significant inhibitory potential with >76 to 89 % inhibition and C3, C4, C6 and C7 demonstrated the highest inhibition of RBD.

Conclusion: The current findings suggest that compounds C3 and C6 effectively disrupt the function of RBD of SARS-CoV-2 spike protein and can serve as potential drug candidates for spike protein.

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boswell酸衍生分子作为SARS-CoV-2刺突蛋白抑制剂：综合虚拟筛选、三重分子动态模拟和生化验证

背景：冠状病毒病（COVID-19）是由SARS-CoV-2引起的高传染性疾病。SARS-CoV-2刺突蛋白与人ACE2受体结合，促进病毒进入宿主细胞；因此，刺突蛋白是药物开发的潜在靶点。目的：考虑到SARS-CoV-2刺突蛋白对病毒复制的重要意义，本研究确定了有效的SARS-CoV-2刺突蛋白抑制剂，以对抗病毒感染。方法：在目前的研究中，我们使用基于结构的虚拟方法筛选了大约900种天然和合成的抗刺突蛋白受体结合域（RBD）的化合物，然后进行了体外抑制生物测定。结果：共鉴定出7个（c1 ~ c7）强效化合物，对接评分≥-6.66 Kcal/mol；它们的药物相似性、药代动力学和药效学特性优良，无毒副作用。这些分子进行了200 ns的三次模拟，进一步证实了它们与RBD的稳定结合。计算的结合自由能反映了配合物的紧密包裹，C4、C7和C6的结合自由能高于C1- c3，而预测的熵能显示C4、C7和C1的值高于其他化合物，表明C4、C7和C1的结合引起了刺突蛋白的构象变化，从而提高了蛋白质的热力学稳定性。这些计算分析后来通过体外生物测定验证。值得注意的是，C2-C7表现出明显的抑制潜力，抑制率为>76 ~ 89%，C3、C4、C6和C7对RBD的抑制作用最高。结论：化合物C3和C6可有效破坏SARS-CoV-2刺突蛋白的RBD功能，可作为刺突蛋白的潜在候选药物。

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

Current medicinal chemistry 医学-生化与分子生物学

CiteScore

8.60

自引率

2.40%

发文量

468

审稿时长

3 months

期刊介绍： Aims & Scope Current Medicinal Chemistry covers all the latest and outstanding developments in medicinal chemistry and rational drug design. Each issue contains a series of timely in-depth reviews and guest edited thematic issues written by leaders in the field covering a range of the current topics in medicinal chemistry. The journal also publishes reviews on recent patents. Current Medicinal Chemistry is an essential journal for every medicinal chemist who wishes to be kept informed and up-to-date with the latest and most important developments.