Molecular targets and mechanisms of Guanxinning tablet in treating atherosclerosis: Network pharmacology and molecular docking analysis

Chaofeng Niu; Peiyu Zhang; Lijing Zhang; Dingfeng Lin; Haixia Lai; Di Xiao; Yong Liu; Rui Zhuang; Meng Li; Liyong Ma; Jiaqi Ye; Yi Pan

doi:10.1097/MD.0000000000035106

Molecular targets and mechanisms of Guanxinning tablet in treating atherosclerosis: Network pharmacology and molecular docking analysis

Medicine (Baltimore). 2023 Sep 29;102(39):e35106. doi: 10.1097/MD.0000000000035106.

Authors

Chaofeng Niu¹, Peiyu Zhang, Lijing Zhang, Dingfeng Lin, Haixia Lai, Di Xiao, Yong Liu, Rui Zhuang, Meng Li, Liyong Ma, Jiaqi Ye, Yi Pan

Affiliation

¹ Department of Cardiology, Dongzhimen Hospital, Beijing University of Chinese Medicine, Beijing, China.

Abstract

Background: Guanxinning tablet (GXNT), a Chinese patent medicine, is composed of salvia miltiorrhiza bunge and ligusticum striatum DC, which may play the role of endothelial protection through many pathways. We aimed to explore the molecular mechanisms of GXNT against atherosclerosis (AS) through network pharmacology and molecular docking verification.

Methods: The active ingredients and their potential targets of GXNT were obtained in traditional Chinese medicine systems pharmacology database and analysis platform and bioinformatics analysis tool for molecular mechanism of traditional Chinese medicine databases. DrugBank, TTD, DisGeNET, OMIM, and GeneCards databases were used to screen the targets of AS. The intersection targets gene ontology and Kyoto encyclopedia of genes and genomes enrichment analysis were performed in DAVID database. GXNT-AS protein-protein interaction network, ingredient-target network and herb-target-pathway network were constructed by Cytoscape. Finally, we used AutoDock for molecular docking.

Results: We screened 65 active ingredients of GXNT and 70 GXNT-AS intersection targets. The key targets of protein-protein interaction network were AKT1, JUN, STAT3, TNF, TP53, IL6, EGFR, MAPK14, RELA, and CASP3. The Kyoto encyclopedia of genes and genomes pathway enrichment analysis showed that pathways in cancer, lipid and atherosclerosis, and PI3K-Akt signaling pathway were the main pathways. The ingredient-target network showed that the key ingredients were luteolin, tanshinone IIA, myricanone, dihydrotanshinlactone, dan-shexinkum d, 2-isopropyl-8-methylphenanthrene-3,4-dione, miltionone I, deoxyneocryptotanshinone, Isotanshinone II and 4-methylenemiltirone. The results of molecular docking showed that tanshinone IIA, dihydrotanshinlactone, dan-shexinkum d, 2-isopropyl-8-methylphenanthrene-3,4-dione, miltionone I, deoxyneocryptotanshinone, Isotanshinone II and 4-methylenemiltirone all had good binding interactions with AKT1, EGFR and MAPK14.

Conclusion: The results of network pharmacology and molecular docking showed that the multiple ingredients within GXNT may confer protective effects on the vascular endothelium against AS through multitarget and multichannel mechanisms. AKT1, EGFR and MAPK14 were the core potential targets of GXNT against AS.

MeSH terms

Atherosclerosis* / drug therapy
Drugs, Chinese Herbal* / pharmacology
Drugs, Chinese Herbal* / therapeutic use
ErbB Receptors
Humans
Mitogen-Activated Protein Kinase 14*
Molecular Docking Simulation
Network Pharmacology
Phosphatidylinositol 3-Kinases

Substances

tanshinone
Mitogen-Activated Protein Kinase 14
Phosphatidylinositol 3-Kinases
ErbB Receptors
Drugs, Chinese Herbal