[1]杨杰 彭启伦 郭步伐 丁维俊.半夏-附子药对拮抗冠心病分子机制研究[J].现代中医药,2022,1(02):054-62.[doi:10.13424/j.cnki.mtcm.2022.02.010]
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半夏-附子药对拮抗冠心病分子机制研究
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《现代中医药》[ISSN:1006-6977/CN:61-1281/TN]

卷:
1
期数:
2022年02期
页码:
054-62
栏目:
方药纵横
出版日期:
2022-04-16

文章信息/Info

文章编号:
1672-0571(2022)02-0054-09
作者:
杨杰1 彭启伦1 郭步伐1 丁维俊2
1.毕节医学高等专科学校基础医学系,贵州 毕节 551700;
2.成都中医药大学基础医学院,四川 成都 610075
关键词:
关键词:网络药理学半夏-附子药对冠心病成分-靶点-通路分子机制
分类号:
R256.22
DOI:
10.13424/j.cnki.mtcm.2022.02.010
文献标志码:
A
摘要:
摘 要:目的 通过网络药理学与分子对接方法探讨半夏-附子同方配伍拮抗冠心病的分子机制。方法 基于TCMSP、DisGeNET和OMIM等多个数据库查询半夏-附子药对活性成分和冠心病相关靶点。采用STRING数据库构建半夏-附子药对活性成分拮抗冠心病相关靶点PPI网络,运用Cytoscape3.7.1软件构建“半夏-附子药对活性成分-冠心病-靶点-通络”网络,随后使用R语言脚本进行GO和KEGG通路富集分析,最后进行分子对接验证。结果 半夏-附子药对活性成分16个,与半夏-附子同方配伍拮抗冠心病的相关靶点有35个,35个靶点富集在57个GO term上,同时富集在75条KEGG信号转导通路上;KEGG富集P值最显著的信号转导通路为Lipid and atherosclerosis;进一步分析提示了,半夏-附子药对活性成分拮抗冠心病的核心靶点可能为AKT1、FOS、MMP9和PTGS2,其关键有效成分为baicalein、cavidine和deltoin。结论 本研究初步揭示了半夏-附子药对活性成分通过调控Lipid and atherosclerosis信号转导通路而拮抗冠心病,为半夏-附子药对抗冠心病的物质基础及分子机制的进一步研究奠定了理论基础。

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备注/Memo

备注/Memo:
基金项目:贵州省科技计划(黔科合基础[2019]1003)
更新日期/Last Update: 2022-04-08