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首页> 外文期刊>RSC Advances >Prediction of the targets of the main components in blood after oral administration of Xanthii Fructus: a network pharmacology study
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Prediction of the targets of the main components in blood after oral administration of Xanthii Fructus: a network pharmacology study

机译:口服黄原胶后血液中主要成分目标的预测:一项网络药理研究

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Xanthii Fructus (XF), a famous traditional Chinese medicine (TCM), has been widely used in the treatment of rhinitis and other diseases. However, the targets of the main XF components found in the blood after oral administration of XF extract are still unclear. In the current study, a feasible systems pharmacology method was developed to predict these targets. In accordance with our previous research, XF components were selected including cleomiscosin A, myristic acid, succinic acid, xanthosine, sitostenone, emodin, apigenin, and chrysophanol. Three components, namely emodin, apigenin, and chrysophanol, failed to be detected with target proteins, thus the other five components, namely cleomiscosin A, myristic acid, succinic acid, xanthosine and sitostenone, were eventually chosen for further systematic analysis. Ninety-nine target proteins and fifty-two pathways were found after a series of analyses. The frequency of some target proteins was much higher than that of others; high frequencies were obtained for P15086, P07360, P07195, MAOM_HUMAN (P23368), P35558, P35520, ACE_HUMAN (P12821), C1S_HUMAN (P09871), PH4H_HUMAN (P00439), FPPS_HUMAN (P14324), P50613, P12724, IMPA1_HUMAN (P29218), HXK1_HUMAN (P19367), P14061, and MCR_HUMAN (P08235). The frequency of eight pathways was also high, including Generic Transcription Pathway, RNA Polymerase II Transcription, Metabolism, Metabolism of steroids, Gene expression (Transcription), Cellular responses to stress, Platelet activation, signaling and aggregation, Signaling by Receptor Tyrosine Kinases, and Cellular Senescence. This study identified a common pathway – the Metabolism pathway – for all five XF components. We successfully developed a network pharmacology method to predict the potential targets of the main XF components absorbed in serum after oral administration of XF extract.
机译:Xanthii Fructus(XF)是一种著名的中药(TCM),已被广泛用于治疗鼻炎和其他疾病。但是,口服XF提取物后血液中主要XF成分的目标仍不清楚。在当前的研究中,开发了一种可行的系统药理方法来预测这些目标。根据我们先前的研究,选择了XF成分,包括粘菌素A,肉豆蔻酸,琥珀酸,黄嘌呤,西妥烯酮,大黄素,芹菜素和菜豆酚。未能用靶蛋白检测出大黄素,芹菜素和chrysophanol这三个成分,因此最终选择了另外五个五个成分,分别是粘粘素A,肉豆蔻酸,琥珀酸,黄嘌呤和西妥烯酮,以进行进一步的系统分析。经过一系列分析,发现了九十九个靶蛋白和五十二个途径。一些靶蛋白的频率远高于其他靶蛋白的频率。对于P15086,P07360,P07195,MAOM_HUMAN(P23368),P35558,P35520,ACE_HUMAN(P12821),C1S_HUMAN(P09871),PH4H_HUMAN(P00439),FPPS_HUMAN(P14324),P50613,P12724,KX18(HUM) (P19367),P14061和MCR_HUMAN(P08235)。八个途径的频率也很高,包括通用转录途径,RNA聚合酶II转录,代谢,类固醇代谢,基因表达(转录),细胞对应激的反应,血小板活化,信号传导和聚集,受体酪氨酸激酶信号传导以及细胞衰老。这项研究确定了XF的所有五个成分的共同途径-代谢途径。我们成功开发了一种网络药理学方法,可以预测口服XF提取物后吸收到血清中的主要XF成分的潜在目标。

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