马蹄莲96%乙醇提取物中化合物的预测。增加雌激素受体-α激活的叶片

Burhan Ma’arif, F. A. Muslikh, Destiya Argo Pamuji Fihuda, S. Syarifuddin, B. Fauziyah
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引用次数: 4

摘要

经历更年期的女性会经历雌激素缺乏,这会影响她们的健康,其中之一会增加神经退行性疾病的风险。马蹄莲植物雌激素化合物在与其受体或er依赖途径结合后可提供活性。本研究采用ERα (1A52)受体的分子对接方法在硅片上进行。对前人研究中提取的水仙叶96%乙醇提取物的代谢物谱化合物进行了硅晶分析。使用Biovia Discovery Studio 2021应用程序进行样品制备,分离大分子和天然配体,并使用ChemDraw Ultra 12.0准备获得3D结构。然后利用SwissADME网络工具分析其药代动力学和药效学。此外,利用Avogadro 1.0.1优化化合物的几何结构,并利用Autodock vina (PyRx 0.8)进行化合物与1A52受体的分子对接。交互可视化阶段使用Biovia Discovery Studio 2021进行,毒性测试使用ProTox II在线工具进行。结果表明,6个化合物符合药代动力学和药效学标准,毒性,药效团距离和氨基酸结合与天然17β-雌二醇相似,17β-雌二醇是一种具有抗神经炎症作用的1A52激动剂。因此,96%乙醇提取物可通过抗神经炎症机制抑制帕金森病的进展。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Prediction of Compounds from 96% Ethanol Extract of Marsilea crenata Presl. Leaves in Increasing Estrogen Receptor-α Activation
Women who experience menopause will experience estrogen deficiency, which will impact their health, one of which will increase the risk of neurodegenerative. Phytoestrogen compounds in Marsilea crenata can provide activity after binding to their receptors or ER-dependent pathways. The research was conducted in silico with the molecular docking method using the ERα (1A52) receptor. In silico analysis was carried out on the metabolite profiling compound of the 96% ethanol extract of M. crenata leaves from the previous study. Sample preparation was carried out using the Biovia Discovery Studio 2021 application to separate macromolecules and native ligands and prepared to get a 3D structure using ChemDraw Ultra 12.0. then analyzed its pharmacokinetics and pharmacodynamics with the SwissADME webtool. Furthermore, the geometry of the compound was optimized using Avogadro 1.0.1, and molecular docking of the compound to the 1A52 receptor was carried out using Autodock vina (PyRx 0.8). The interaction visualization stage was carried out with Biovia Discovery Studio 2021, and a toxicity test was carried out using the ProTox II online tool. The results of the in-silico study showed that six compounds met the pharmacokinetic and pharmacodynamic criteria, toxicity, and had similar pharmacophore distances and amino acid binding with native 17β-estradiol, a 1A52 agonist with anti-neuroinflammatory effect. So, 96% ethanol extract of M. crenata leaves is predicted to potentially inhibit PD progression with an anti-neuroinflammatory mechanism.
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