Anti-platelet aggregation mechanism of Xixian Tongshuan Preparation based on molecular simulation methods.
10.19540/j.cnki.cjcmm.20190111.005
- Author:
Bo-Wen ZHAO
1
;
Xiao-Hua ZHANG
1
;
Yu GU
1
;
Shuai ZHAO
1
;
Xi CHEN
1
;
Yin-Zhen LUO
1
;
Yan-Ling ZHANG
1
Author Information
1. State Laboratory of Traditional Chinese Medicine Information Engineering,State Administration of Traditional Chinese Medicine,School of Chinese Material Medica,Beijing University of Chinese Medicine Beijing 100102,China.
- Publication Type:Journal Article
- Keywords:
Xixian Tongshuan Preparation;
anti-platelet aggregation;
molecular docking;
pharmacophore;
virtual screening
- MeSH:
Databases, Pharmaceutical;
Drugs, Chinese Herbal;
pharmacology;
Humans;
Molecular Docking Simulation;
Platelet Aggregation;
Platelet Aggregation Inhibitors;
pharmacology;
Thrombosis
- From:
China Journal of Chinese Materia Medica
2019;44(9):1882-1888
- CountryChina
- Language:Chinese
-
Abstract:
The thrombus is a deposit that is formed on the surface of the endovascular or at the site of repair,and known as the main complication of cardiovascular disease and the cause of death. At the same time,thrombus is mainly treated by the following three ways: anticoagulation,anti-platelet aggregation and thrombolysis. In this study,the chemical constituents of seven traditional Chinese medicines in the Xixian Tongshuan Preparation were collected to construct a component database. Subsequently,the pharmacophore were used to screen out the component database,and molecular docking was used to screen out the results of pharmacophore for explaining the material basis and mechanism that Xixian Tongshuan Preparation exerts anti-thrombotic activity by inhibiting platelet aggregation. First of all,P2 Y12,GPⅡb/Ⅲa and PAR1 were selected as study vectors,the optimal models of inhibitors were obtained respectively through verification and evaluation of the pharmacophore models. Afterwards,the component database was screened out by the optimal pharmacophore models of PAR1,P2 Y12 and GP Ⅱ b/Ⅲ a,and the molecular docking method was used to further refine the screening results. The screening results indicated that the anti-platelet aggregation effect of Xixian Tongshuan Preparation was correlated with the inhibition of P2 Y12,PAR1 and GPⅡb/Ⅲa expressions with saffower yellower,hirudin and candidin and notoginseng triterpenes,folinic acid,respectively. The material basis and mechanism of anti-platelet aggregation of Xixian Tongshuan Preparation provided a theoretical basis for the clinical use of the preparation and the lead compounds for the development of anti-platelet aggregation drugs.