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A network pharmacology approach to determine the underlying mechanisms of action of Yishen Tongluo formula for the treatment of oligoasthenozoospermia

机译:一种网络药理学方法,以确定宜寿通络公式治疗寡孢菌菌治疗的潜在作用机制

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Oligoasthenozoospermia is a complex disease caused by a variety of factors, and its incidence is increasing yearly worldwide. Yishen Tongluo formula (YSTLF), created by Professor Sun Zixue, has been used to treat oligoasthenozoospermia in clinical practice for several decades with a good therapeutic effect. However, the chemical and pharmacological profiles of YSTLF remain unclear and need to be elucidated. In this study, a network pharmacology approach was applied to explore the potential mechanisms of YSTLF in oligoasthenozoospermia treatment. All of the compounds in YSTLF were retrieved from the corresponding databases, and the bioactive ingredients were screened according to their oral bioavailability (OB) and drug-likeness (DL). The potential proteins of YSTLF were obtained from the traditional Chinese medicine systems pharmacology (TCMSP) database and the Bioinformatics Analysis Tool for Molecular Mechanism of Traditional Chinese Medicine (BATMAN-TCM) database, while the potential genes of oligoasthenozoospermia were obtained from the GeneCards database and the DisGeNET database. The STRING database was used to construct an interaction network according to the common targets identified by the online tool Venny for YSTLF and oligoasthenozoospermia. The topological characteristics of nodes were visualized and analyzed through Cytoscape. Biological functions and significant pathways were determined and analyzed using the Gene Ontology (GO) knowledgebase, the Kyoto Encyclopedia of Genes and Genomes (KEGG) and Metascape. Finally, the disease-formula-compound-target-pathway network was constructed by Cytoscape. A total of 106 bioactive ingredients and 134 potential targets from YSTLF were associated with oligoasthenozoospermia or considered to be therapeutically relevant. Pathway analysis indicated that the PI3K/Akt, MAPK and apoptosis signaling pathways were significant pathways involved in oligoasthenozoospermia. In conclusion, the current study expounded the pharmacological actions and molecular mechanisms of YSTLF in treating oligoasthenozoospermia from a holistic viewpoint. The potential molecular mechanisms were closely related to antioxidative stress, antiapoptosis and anti-inflammation, with TNF, CCND1, ESR1, NFKBIA, NR3C1, MAPK8, and IL6 being possible targets. This network pharmacology prediction may offer a helpful tool to illustrate the molecular mechanisms of the Chinese herbal compound YSTLF in oligoasthenozoospermia treatment.
机译:Oligoasthenoospermia是由各种因素引起的复杂疾病,其发病率在全世界的每年增加。由孙紫川教授创建的伊什通络配方(YSTLF)已被用于治疗寡血管孢子患者在临床实践中进行了几十年,具有良好的治疗效果。然而,YSTLF的化学和药理学谱仍然不清楚并且需要阐明。在本研究中,应用了网络药理学方法,探讨了YSTLF在寡核苷酸治疗中的潜在机制。从相应的数据库中检出YSTLF中的所有化合物,并根据其口服生物利用度(OB)和药物象征(DL)筛选生物活性成分。 YSTLF的潜在蛋白质是从中药系统药理学(TCMSP)数据库和用于中医(BATMAN-TCM)数据库的分子机制的生物信息学分析工具,而来自Genecards数据库的寡核苷酸血症患者的潜在基因DISGENET数据库。字符串数据库用于根据YSTLF和OligoasthenoSpermia的在线工具venny识别的常见目标来构建交互网络。节点的拓扑特征通过Cytoscape进行了可视化和分析。使用基因本体(GO)知识库,基因和基因组(KEGG)和FEARASCAPE的基因本体(GO)知识库,确定并分析生物功能和显着的途径。最后,通过Cytoscape构建疾病 - 配方复合靶途径网络。总共106种生物活性成分和来自YSTLF的134个潜在靶标与寡血管孢子症有关,或被认为是治疗性相关的。途径分析表明,PI3K / AKT,MAPK和凋亡信号传导途径是寡孢子瘤患者的显着途径。总之,目前的研究阐述了YSTLF从整体观点治疗寡孢子瘤的药理作用和分子机制。潜在的分子机制与抗氧化应激,抗痘病和抗炎,TNF,CCND1,ESR1,NFKBIA,NR3C1,MAPK8和IL6是可能的靶标的靶标。该网络药理学预测可以提供有用的工具,以说明中草原植物治疗中药化合物YSTLF的分子机制。

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