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摘要:
High-throughput metabolomics can clarify the underlying molecular mechanism of diseases via the quafitative and quantitative analysis of metabofites.This study used the established Yang Huang syndrome (YHS)mouse model to evaluate the efficacy of geniposide (GEN).Urine metabolic data were quantified by ultra-performance liquid chromatography-tandem mass spectrometry.The non-target screening of the massive biological information dataset was performed,and a total of 33 metabolites,including tyramine glucuronide,aurine,and L-cysteine,were identified relating to YHS.These differential metabolites directly participated in the disturbance of phase I reaction and hydrophilic transformation of bilirubin.Interestingly,they were completely reversed by GEN.While,as the auxiliary technical means,we also focused on the molecular prediction and docking results in network pharmacological and integrated analysis part.We used integrated analysis to communicate the multiple results of metabolomics and network pharmacology.This study is the first to report that GEN indirectly regulates the metabolite "tyramine glucuronide" through its direct effect on the target heme oxygenase 1 in vivo.Meanwhile,heme oxygenase-1,a prediction of network pharmacology,was the confirmed metabolic enzyme of phase I reaction in hepatocytes.Our study indicated that the combination of high-throughput metabolomics and network pharmacology is a robust combination for deciphering the pathogenesis of the traditional Chinese medicine (TCM) syndrome.
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篇名 High-throughput metabolomics reveals the perturbed metabolic pathways and biomarkers of Yang Huang syndrome as potential targets for evaluating the therapeutic effects and mechanism of geniposide
来源期刊 医学前沿 学科
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年,卷(期) 2020,(5) 所属期刊栏目 Research Articles
研究方向 页码范围 651-663
页数 13页 分类号
字数 语种 英文
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相关学者/机构
期刊影响力
医学前沿
双月刊
2095-0217
11-5983/R
北京市朝阳区惠新东街4号富盛大厦15层
eng
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990
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0
总被引数(次)
3051
期刊文献
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