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A Network Pharmacology-Based Study on the Hepatoprotective Effect of Fructus Schisandrae

机译:基于网络药理学的五味子保肝作用的研究

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摘要

Fructus schisandrae (Wuweizi in Chinese), a common traditional Chinese herbal medicine, has been used for centuries to treat chronic liver disease. The therapeutic efficacy of Wuweizi has also been validated in clinical practice. In this study, molecular docking and network analysis were carried out to explore the hepatoprotective mechanism of Wuweizi as an effective therapeutic approach to treat liver disease. Multiple active compounds of Wuweizi were docked with 44 protein targets related with viral hepatitis, fatty liver, liver fibrosis, cirrhosis, and liver cancer. A compound–target network was constructed through network pharmacology analysis, predicting the relationships of active ingredients to the targets. Our results demonstrated that schisantherin, schisandrin B, schisandrol B, kadsurin, Wuweizisu C, Gomisin A, Gomisin G, and angeloylgomisin may target with 21 intracellular proteins associated with liver diseases, especially with fatty liver disease. The CYP2E1, PPARα, and AMPK genes and their related pathway may play a pivotal role in the hepatoprotective effects of Wuweizi. The network pharmacology strategy used provides a forceful tool for searching the action mechanism of traditional herbal medicines and novel bioactive ingredients.
机译:五味子(一种常见的中草药)已被用于治疗慢性肝病已有好几个世纪了。无味子的疗效也已在临床实践中得到验证。本研究通过分子对接和网络分析,探讨了五味子的保肝作用,作为治疗肝病的有效方法。无味子的多种活性化合物与44种与病毒性肝炎,脂肪肝,肝纤维化,肝硬化和肝癌有关的蛋白质靶标对接。通过网络药理分析构建了化合物-靶标网络,预测了活性成分与靶标之间的关系。我们的结果表明,五味子素,五味子素B,五味子酚B,kadsurin,无味子素C,Gomisin A,Gomisin G和Angeloylgomisin可能靶向21种与肝脏疾病(尤其是脂肪肝疾病)相关的细胞内蛋白。 CYP2E1,PPARα和AMPK基因及其相关途径可能在五味子的保肝作用中起着关键作用。使用的网络药理学策略为搜索传统草药和新型生物活性成分的作用机理提供了有力的工具。

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