Mechanism of Sangqi Qingxuan Liquid in Alleviating Vascular Endothelial Injury in Hypertension Focuses on β-Catenin

REN Wei-quan; ZENG Xin; LIAO Jiang-quan; HUANG Li; LI Lin

doi:10.1007/s11655-025-4013-8

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Mechanism of Sangqi Qingxuan Liquid in Alleviating Vascular Endothelial Injury in Hypertension Focuses on β-Catenin

Original Article | Updated：2025-07-30

- Mechanism of Sangqi Qingxuan Liquid in Alleviating Vascular Endothelial Injury in Hypertension Focuses on β-Catenin
- Chinese Journal of Integrative Medicine Vol. 31, Issue 8, Pages: 726-734(2025)
- Affiliations：
  
  1.Department of Traditional Chinese Medicine, Xuanwu Hospital Capital Medical University, Beijing (100053), China
  2.Department of Education, Xuanwu Hospital Capital Medical University, Beijing (100053), China
  3.Department of Integrated Chinese and Western Medicine Cardiology, China-Japan Friendship Hospital, Beijing (100029), China
- Author bio：
  
  Associate Prof. LI Lin, E-mail: lilinxcy@126.com
- Funds：
- DOI：10.1007/s11655-025-4013-8
  CLC：
- Accepted：24 February 2025，
  
  Published Online：13 June 2025，
  
  Published：2025-08
- Accepted：
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REN Wei-quan, ZENG Xin, LIAO Jiang-quan, et al. Mechanism of Sangqi Qingxuan Liquid in Alleviating Vascular Endothelial Injury in Hypertension Focuses on β-Catenin[J]. Chinese journal of integrative medicine, 2025, 31(8): 726-734.
DOI：

REN Wei-quan, ZENG Xin, LIAO Jiang-quan, et al. Mechanism of Sangqi Qingxuan Liquid in Alleviating Vascular Endothelial Injury in Hypertension Focuses on β-Catenin[J]. Chinese journal of integrative medicine, 2025, 31(8): 726-734. DOI： 10.1007/s11655-025-4013-8.

摘要

目的:

基于网络药理学探讨桑杞清眩液治疗高血压主动脉血管内皮细胞 (arterial vascular endothelial cells

AVECs) 损伤的主要成分及其潜在机制.

方法:

运用中药系统药理学与分析平台 (Traditional Chinese Medicine Systems Pharmacology and Analysis Platform

TCMSP) 和中医药综合数据库 (Traditional Chinese Medicine Integrated Database

TCMID) 筛选出桑杞清眩液 (Sangqi Qingxuan Liquid

SQQX) 符合口服利用度和药物相似性标准的活性成分

采用Cytoscape 3.6软件构建活性成分-靶点网络

相互作用基因/蛋白质检索工具 (Search Tool for the Retrieval of Interacting Genes/Proteins

STRING) 数据库构建SQQX治疗高血压相关靶点的蛋白质相互作用 (protein-protein interaction

PPI) 网络. 利用Metascape数据库对PPI网络中的蛋白质进行基因本体论 (gene ontology

GO) 生物学功能富集分析和MSigDB通路富集分析

并采用UPLC-MS对SQQX的主要成分进行分析. 进一步基于网络药理学结果

通过慢病毒转染Wnt/β-catenin信号通路关键因子验证SQQX改善高血压内皮细胞损伤的作用机制. 使用血管紧张素Ⅱ (angiotensin Ⅱ

Ang Ⅱ) 诱导AVECs建立高血压内皮功能损伤模型

测定细胞活力、细胞内一氧化氮含量、丙二醛含量及超氧化物歧化酶活性

确定最佳诱导条件. 以细胞活力、细胞DNA活性为指标

采用梯度法确定SQQX最佳干预条件. 将细胞分为空白组、模型组、过表达慢病毒阴性对照组、过表达慢病毒组、过表达慢病毒+SQQX干预 (2.47 mg/mL

12 h) 组、抑制慢病毒阴性对照组、抑制慢病毒组、抑制慢病毒+SQQX干预 (2.47 mg/mL

12 h) 组. 最后采用实时荧光定量PCR和Western blotting分析SQQX调控Wnt/β-catenin信号通路的分子机制.

结果:

SQQX主要成分从高到低依次为甜菜碱、蒙花苷、绿原酸

网络药理学分析筛选出12条与高血压血管内皮相关的通路. 经过检测发现

1μmol/L AngⅡ作用12 h为诱导AVECs损伤的最佳条件

2.47 mg/mL SQQX干预12 h为治疗AVECs损伤的最佳条件. 基于Wnt/β-catenin信号通路相互作用网络的实验验证中

SQQX可显著降低β-catenin过表达慢病毒引起的β-catenin、Smad2、过氧化物酶体增殖物激活受体 (peroxisome proliferator-adivated receptors

PPARs) 、内皮型一氧化氮合酶 (endothelial nitric oxide synthase

eNOS) 、内皮素-1 (endothelin-1

ET-1) 的表达 (

0.05或

0.01) . β-catenin抑制慢病毒即可改善血管内皮细胞功能

进一步SQQX干预后未观察到明显变化.

结论:

SQQX可能通过调控Wnt/β-catenin信号通路来保护AVECs损伤.

Abstract

Objective:

To explore the main components and potential mechanisms of Sangqi Qingxuan Liquid in the treatment of arterial vascular endothelial cells (AVECs) injury in hypertension through network pharmacology.

Methods:

Traditional Chinese Medicine Systems Pharmacology and Analysis Platform (TCMSP) and Traditional Chinese Medicine Integrated Database (TCMID) were used to screen the active components of Sangqi Qingxuan Liquid (SQQX)

which met the oral utilization rate and drug similarity criteria. An active component-target network was constructed using Cytoscape 3.6 software. A protein-protein interaction (PPI) network of targets associated with SQQX treatment for hypertension was constructed using the Search Tool for the Retrieval of Interacting Genes/Proteins (STRING) database. The Metascape database was used to perform enrichment analysis of gene ontology biological functions and MSigDB pathway enrichment analysis of proteins in the PPI network. Further analysis of the main components of SQQX was performed using UPLC-MS. Based on the results of network pharmacology

the mechanism of SQQX to improve the injury of AVECs in hypertension was verified through lentiviral transfection by Wnt/β-catenin signaling pathway. AVECs induced by angiotensin Ⅱ (Ang Ⅱ) was used to establish a model of endothelial function injury in hypertension. Cell viability

intracellular nitric oxide content

malonaldehyde content

and superoxide dismutase activity were measured to determine the optimal induction conditions. The optimal intervention conditions for SQQX were determined based on cell viability

cellular DNA activity

and the gradient method. The cells were further divided into blank

model

overexpression lentivirus negative control

overexpression lentivirus

overexpression lentivirus + SQQX intervention (2.47 mg/mL

12 h)

inhibition lentivirus negative control

inhibition lentivirus

and inhibition lentivirus + SQQX intervention (2.47 mg/mL

12 h) groups. Finally

quantitative real-time PCR and Western blotting were performed to analyze the molecular mechanisms of SQQX in the Wnt/β-catenin signaling pathway.

Results:

The main SQQX components were betaine

buddleoside

and chlorogenic acid

in descending order. Network pharmacology analysis screened 12 pathways associated with the hypertensive vascular endothelium. The results showed that 1 μmol/L for 12 h was the optimal condition for Ang Ⅱ to induce AVECs injury

and 2.47 mg/mL SQQX intervention for 12 h was the optimal condition for treating AVECs injury. In the experimental validation based on the interaction network of the Wnt/β-catenin signaling pathway

SQQX significantly decreased the expressions of β-catenin

Smad2

peroxisome proliferator-activated receptors (PPARs)

endothelial nitric oxide synthase (eNOS)

and endothelin-1 (ET-1) caused by the β-catenin overexpression lentivirus (

0.05 or

0.01). The function of vascular endothelial cells can be improved by the β-catenin inhibition lentivirus

and no obvious changes were observed after further intervention with SQQX.

Conclusion:

SQQX may protect against AVECs injury by regulating the Wnt/β-catenin signaling pathway.

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