Network Pharmacology Analysis and Biological Validation Systemically Identified the Active Ingredients and Molecular Targets of Kudzu Root on Osteoporosis

被引:0
作者
Liu, Zhi-Wen [1 ,2 ]
Zhang, Bo-Bo [3 ]
Kwok, Kevin Wing-Hin [1 ,2 ]
Dong, Xiao-Li [1 ,2 ]
Wong, Ka-Hing [1 ,2 ]
机构
[1] Hong Kong Polytech Univ, Res Inst Future Food, Hong Kong, Peoples R China
[2] Hong Kong Polytech Univ, Dept Food Sci & Nutr, Hong Kong, Peoples R China
[3] Shantou Univ, Coll Sci, Dept Biol, Guangdong Prov Key Lab Marine Biotechnol, Shantou 515063, Peoples R China
关键词
Kudzu root; osteoporosis; network pharmacology; TNF signaling pathway; NF-kappa B; p38; MAPK; INTEGRATING INFORMATION; RECEPTOR ACTIVATOR; DIFFERENTIATION; RANKL; BONE; OSTEOCLASTOGENESIS; PROLIFERATION; GENES; COUMESTROL; PROTEINS;
D O I
10.3390/ijms26031202
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
As a traditional medicinal food, Kudzu root (KR) has been proven to be an effective medicine for treating osteoporosis (OP). However, its precise targets and underlying integrated pharmacological mechanisms on OP have not yet been systematically investigated. The aim of the present study was to systemically explore the active ingredients, molecular targets, and ingredient-target network of KR against OP by the methods of network pharmacology followed by biological validation in a glucocorticoid-induced bone loss model of zebrafish. Our results identified a total of 15 active compounds with good pharmacokinetic properties in KR and 119 targets related to OP from correspondent databases, forming an ingredient-target network. Additionally, the protein-protein interaction (PPI) network further identified 39 core targets. Enrichment analyses with functional annotation revealed that the TNF signaling pathway and osteoclast differentiation process were significantly enriched by multi-targets including AKT1, P65, MAPK14, JUN, TNF-alpha, MMP9, IL6, and IL1B, etc., and served as the critical targets for molecular docking, molecular dynamics simulation, and in vivo experiment validation. These critical targets performed effectively in molecular docking and molecular dynamics, with AKT1, MMP9, and TNF-alpha exhibiting more prominent binding energy with Coumestrol, Genistein, and Genistein 7-glucoside, respectively. Further experimental validation in a zebrafish model indicated that KR could regulate the expressions of critical targets (AKT1, P65, MAPK14, JUN, TNF-alpha, and MMP9). This study provides a systemic perspective of the relationships between the active ingredients of KR and their multi-targets in OP, thereby constructing a pharmacological network to clarify the mechanisms by which KR ameliorates OP.
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页数:27
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