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An integrated approach for investigating pharmacodynamic material basis of Lingguizhugan Decoction in the treatment of heart failure

药效学 药理学 咖啡酸 代谢组学 汤剂 化学 中医药 山奈酚 传统医学 医学 色谱法 药代动力学 类黄酮 生物化学 抗氧化剂 替代医学 病理
作者
Shuo Sun,Ge Xun,Jia Zhang,Yanhua Gao,Jiachen Ge,Fangfang Liu,Qian Qi,Xin Liu,Yuhuan Tian,Qizhen Sun,Qiao Wang,Xu Wang
出处
期刊:Journal of Ethnopharmacology [Elsevier]
卷期号:295: 115366-115366 被引量:6
标识
DOI:10.1016/j.jep.2022.115366
摘要

As a classical formula of traditional Chinese medicine (TCM), Lingguizhugan Decoction (LGZGD) has been used for treating heart failure (HF) because it has an efficiency of yang-warming and fluid-dispersing. However, the pharmacodynamic material basis of LGZGD responsible for the therapeutic benefits is not well understood.The aim of this study was to elucidate the pharmacodynamic material basis of LGZGD by an integrated approach.Following oral administration of LGZGD in mice, ultra-high performance liquid chromatography-quadrupole time-of-flight mass spectrometry (UHPLC-Q-TOF-MS/MS) was used to identify prototype substances. A heart failure (HF) model was established, followed by an untargeted metabolomics study to determine potential targets of LGZGD. The network pharmacology method was performed to screen substances that interacted with potential targets of LGZGD treating HF. Molecular docking technology was applied to further screen substances based on binding energy. Cell viability assays were conducted to verify pharmacodynamic effects of selected substances.In all, forty-two prototype substances were identified in the blood, urine, and fecal samples of mice. A total of fifty-five differential metabolites were identified using heart tissue untargeted metabolomics. Twenty-five substances of LGZGD were screened relating to thirty-three targets treating HF. Twenty-two substances were filtered according to their binding energy using molecular docking technology. Cell experiments revealed cinnamaldehyde, glycyrrhetinic acid, kaempferol, daidzein, caffeic acid, and catechin could significantly improve the survival rate of H9c2 cells, which might be the pharmacodynamic material basis of LGZGD.A scientific approach that integrated in vivo substances identification, metabolomics, network pharmacology, molecular docking, and cell pharmacodynamic assay has been developed to study the pharmacodynamic material basis of LGZGD in the treatment of HF.
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