Sulistyaning Budi, Annisa Fitri Nurlaila, Icaq Dwi Prasetyo, Indah Nur Rahmadhani, Javier Sebastián, I. Tahir
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引用次数: 2
摘要
受2019冠状病毒病大流行的影响,全球焦虑和抑郁患病率上升了25%。抑郁症可由nNOS酶产生的NO增加引起。没食子酸及其衍生物可从自然界获得,具有多种生物活性。本研究旨在通过结合能值、RMSD值和氨基酸残基特异性结合参数的分子对接方法,确定没食子酸及其衍生物作为nNOS抑制剂的潜力。结果表明,没食子酸、4- o -甲基没食子酸和表没食子儿茶素没食子酸酯的键能为- 1.87;−2.36;和- 0.12 kcal/mol。与标准配体的结合能为−2.84 kcal/mol相比,没食子酸4-O-(6-没食子酰糖苷)的结合能为−4.12 kcal/mol。基于这些结果,没食子酸4-O-(6-没食子酰葡萄糖苷)对nNOS具有潜在的抑制作用。
Molecular Docking of Gallic Acid and Its Derivatives as the Potential nNOS Inhibitors
The global prevalence of anxiety and depression rates have increased by 25% due to the impact of the COVID-19 pandemic. Depression can occur due to an increase in NO produced by the nNOS enzyme. Gallic acid and its derivatives can be obtained from nature and have various biological activities. This study aimed to determine the potential of gallic acid and its derivatives as nNOS inhibitors using the molecular docking method with parameters of binding energy values, RMSD values, and specific binding to amino acid residues. The results showed that gallic acid, 4-O-methyl gallic acid, and epigallocatechin gallate had bond energies of −1.87; −2.36; and −0.12 kcal/mol, respectively. Compared to the standard ligand, which had binding energy of −2.84 kcal/mol, gallic acid 4-O-(6-galloyl glucoside) had binding energy of −4.12 kcal/mol. Based on these results, gallic acid 4-O-(6-galloyl glucoside) can potentially inhibit nNOS.
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