Chrysin Inhibits Indonesian Serotype Foot-and-Mouth-Disease Virus Replication: Insights from DFT, Molecular Docking and Dynamics Analyses

Q4 Agricultural and Biological Sciences Journal of Tropical Biodiversity and Biotechnology Pub Date : 2024-01-08 DOI:10.22146/jtbb.83140
Agus Susilo, M. Cahyati, Nurjannah Nurjannah, D. Pranowo, F. Hermanto, E. P. Primandasari
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Abstract

Chrysin, a predominant compound in Propolis, possesses diverse bioactivities, including antiviral properties. However, its antiviral efficacy against the Indonesian Foot-and-Mouth Disease Virus (FMDV) serotype remains unexplored. This study investigates Chrysin's inhibitory potential against FMDV Indonesian serotype by targeting the 3C Protease (3CP), a vital enzyme for viral replication. Multiple sequence alignment was used to reveal unique characteristics of the Indonesian serotype's 3CP compared to global serotypes. Density Functional Theory (DFT) calculations assessed Chrysin's interaction with 3CP based on electronegativity. Molecular docking and molecular dynamics analyses evaluated Chrysin's inhibitory activity against 3CP, using homology modeling for the Indonesian serotype's 3CP structure. Luteolin, a known FMDV 3CP inhibitor with a similar structure to Chrysin, served as a reference. Results showed distinct 3CP sequences in the Indonesian serotype compared to O serotypes and others. Chrysin exhibited potential electron-donor activity with lower HOMO and LUMO values than Luteolin, but they had similar energy gaps, i.e., 4.016 and 4.044 eV, respectively. Molecular docking indicated similar binding affinities, with Chrysin (-6.365 kcal/mol) and Luteolin (-6.864 kcal/mol) bound to active site residues. Molecular dynamics analysis demonstrated stable 3CP-Chrysin and 3CP-Luteolin complexes, with minor differences in Radius of gyration (Rg) and Root-Mean-Square Fluctuation (RMSF) below 1 Å. From the ligand stability point of view, Chrysin had comparable stability with Luteolin. However, Chrysin formed fewer hydrogen bonds and displayed greater free-binding energy than Luteolin during simulation periods. These findings suggest that Chrysin holds promise as an inhibitor of the Indonesian serotype's FMDV 3C Protease. 
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金黄素抑制印度尼西亚血清型口蹄疫病毒的复制:从 DFT、分子对接和动力学分析中获得的启示
蜂胶中的主要化合物金黄素具有多种生物活性,包括抗病毒特性。然而,它对印尼口蹄疫病毒(FMDV)血清型的抗病毒功效仍有待探索。本研究以病毒复制的重要酶 3C 蛋白酶(3CP)为靶标,研究蛹素对印尼口蹄疫病毒血清型的抑制潜力。多重序列比对揭示了印尼血清型的 3CP 与全球血清型相比的独特特征。密度泛函理论(DFT)计算根据电负性评估了 Chrysin 与 3CP 的相互作用。分子对接和分子动力学分析评估了 Chrysin 对 3CP 的抑制活性,并对印尼血清型的 3CP 结构进行了同源建模。叶黄素是一种已知的 FMDV 3CP 抑制剂,其结构与 Chrysin 相似,可作为参照物。结果显示,与 O 型血清型和其他血清型相比,印尼血清型的 3CP 序列截然不同。金丝桃素具有潜在的电子供体活性,其 HOMO 和 LUMO 值低于木犀草素,但两者的能隙相似,分别为 4.016 和 4.044 eV。分子对接显示了相似的结合亲和力,Chrysin(-6.365 kcal/mol)和 Luteolin(-6.864 kcal/mol)与活性位点残基结合。分子动力学分析表明 3CP-Chrysin 和 3CP-Luteolin 复合物非常稳定,回转半径(Rg)和均方根波动(RMSF)在 1 Å 以下略有不同。不过,在模拟期间,与木犀草素相比,菊黄素形成的氢键更少,显示的自由结合能更大。这些发现表明,金丝桃素有望成为印尼血清型 FMDV 3C 蛋白酶的抑制剂。
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
Journal of Tropical Biodiversity and Biotechnology
Journal of Tropical Biodiversity and Biotechnology Immunology and Microbiology-Applied Microbiology and Biotechnology
CiteScore
1.10
自引率
0.00%
发文量
40
审稿时长
12 weeks
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