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首页> 外文期刊>Evidence-based complementary and alternative medicine: eCAM >Analysis of the Anti-Inflammatory and Analgesic Mechanism of Shiyifang Vinum Based on Network Pharmacology
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Analysis of the Anti-Inflammatory and Analgesic Mechanism of Shiyifang Vinum Based on Network Pharmacology

机译:基于网络药理学的石细致仁抗炎和镇痛机制分析

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Objective . The possible core active compounds and potential mechanism of action of Shiyifang Vinum were explored through network pharmacology and in vitro enzyme activity verification experiments. Methods . We screened the core active components and the action targets of Shiyifang Vinum through the TCMSP database and literature mining and drew a Venn map of the intersection with anti-inflammatory and analgesic-related gene targets. Go and KEGG analyses were enriched with the David database. The compound target pathway network was constructed using Cytoscape 3.6.1. The binding strength of core active compounds and target proteins was verified through molecular docking, and the direct effects of Shiyifang Vinum and four monomer compounds on COX-2 enzyme activity were detected through an in vitro enzyme activity test. Results . 14 active compounds and 11 targets were screened out from Shiyifang Vinum through TCMSP database and literature mining; 252 GO entries were obtained by GO analysis, and 114 signal pathways were screened by KEGG analysis. The results of the molecular docking showed that the core compounds and target proteins had strong binding activity. In vitro validation experiments showed that both the Shiyifang Vinum and the four monomer compounds could inhibit the activity of COX-2. Conclusion . This study preliminarily explored the potential active compounds and target proteins of the anti-inflammatory and analgesic effects of Shiyifang Vinum, which could provide a scientific basis for further study on the anti-inflammatory and analgesic mechanism and material basis of this recipe.
机译:客观的 。通过网络药理学和体外酶活性验证实验探索了石细芳v的可能核心活性化合物和潜在作用机制。方法 。我们通过TCMSP数据库和文献矿业筛选了核心活动成分和石义牧场的动作目标,并用抗炎和镇痛相关基因靶标制定了交叉口的Venn映射。 Go和Kegg分析丰富了David数据库。化合物靶途径网络使用Cytoscape 3.6.1构建。通过分子对接验证了核心活性化合物和靶蛋白的结合强度,通过体外酶活性试验检测Shiyifang vinum和四种单体化合物对COX-2酶活性的直接作用。结果 。通过TCMSP数据库和文献挖掘,从石义章中筛选了14个活性化合物和11个靶点;通过去分析获得252进入,通过KEGG分析筛选114个信号途径。分子对接的结果表明,核心化合物和靶蛋白具有强的结合活性。体外验证实验表明,石义芳樟和四种单体化合物都可以抑制COX-2的活性。结论 。本研究初步探讨了石细芳·乙烯木的抗炎和镇痛作用的潜在活性化合物和靶蛋白,可以为进一步研究这种食谱的抗炎和镇痛机制和物质基础提供科学依据。

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