Computational Investigation of Endophytic Fungal (Penicillium citrinum CGJ-C2) Compound and its In-silico Derivatives on the Inhibition of RNA-dependent RNA Polymerase of SARS-CoV2

Jagadeesha Poyya, Ananda Danagoudar, Chandrasekhar G Joshi, Ajay S Khandagale, Raju N. G
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Abstract

Background: The SARS-CoV2 was responsible for the pandemic situation across the world. SARS-CoV2 is an RNA virus, and its replication depends on RNA Dependent RNA Polymerase (RdRp). Hence, blocking of RdRP would be an alternative strategy to inhibit the virus multiplication without affecting the host physiology. Objective: The current study investigated the inhibitory effect of bioactive compound F3 isolated from P. citrinum CGJ-C2 and its in-silico derivates against RdRp of COVID using computational methods. Methods: Compound F3 and its derivatives were generated computationally, and the crystal structure of RdRp was processed prior to docking. The RdRp and the bioactive compounds were docked using Glide with three levels of precisions. Post-docking MMGBSA analysis and Molecular Dynamic simulations were carried out to study the stability of the docking interactions. Results: Based on the Glide XP score and MMGBSA analysis of fifteen ligands, three leads were selected, compound F3 (-8.655 Kcal/mol), D-1(-8.295 Kcal/mol), and D-14(-8.262 Kcal/mol). These leads (Compound F3, D-1, and D-14) were further evaluated using molecular dynamics (MD) simulation. MD simulations studies showed the stable bonding interaction between LYS500 and ARG569 residues of RdRp with the three lead molecules. Conclusion: Our study highlighted the potential of compounds in terms of binding, interaction stability, and structural integrity. Therefore, these leads can be chosen for further studies in in vitro and in vivo to develop a novel anti-SARS-CoV2 agent with minimal side effects.
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内生真菌(Penicillium citriinum CGJ-C2)化合物及其硅衍生物抑制SARS-CoV2 RNA依赖性RNA聚合酶的计算研究
背景:SARS-CoV2是造成全球疫情的主要原因。SARS-CoV2是一种RNA病毒,其复制依赖于RNA依赖性RNA聚合酶(RdRp)。因此,阻断RdRP可能是抑制病毒增殖而不影响宿主生理的另一种策略。目的:采用计算方法研究从柑橘属植物CGJ-C2中分离的生物活性化合物F3及其硅衍生物对新冠病毒RdRp的抑制作用。方法:通过计算生成化合物F3及其衍生物,对接前对RdRp的晶体结构进行处理。RdRp和生物活性化合物使用Glide进行对接,精度为三个级别。通过对接后MMGBSA分析和分子动力学模拟研究了对接相互作用的稳定性。结果:根据15个配体的Glide XP评分和MMGBSA分析,选择了3个先导化合物F3 (-8.655 Kcal/mol)、D-1(-8.295 Kcal/mol)和D-14(-8.262 Kcal/mol)。这些先导物(化合物F3、D-1和D-14)进一步通过分子动力学(MD)模拟进行评估。MD模拟研究表明,RdRp的LYS500和ARG569残基与三种铅分子之间存在稳定的键相互作用。结论:我们的研究突出了化合物在结合、相互作用稳定性和结构完整性方面的潜力。因此,可以选择这些线索进行进一步的体外和体内研究,以开发一种副作用最小的新型抗sars - cov2药物。
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