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循环微颗粒和动脉粥样硬化中的内皮祖细胞:厄贝沙坦的药理作用。

Circulating microparticles and endothelial progenitor cells in atherosclerosis: pharmacological effects of irbesartan.

机构信息

Petru Poni' Institute of Macromolecular Chemistry, Iasi, Romania.

出版信息

J Thromb Haemost. 2012 Apr;10(4):680-91. doi: 10.1111/j.1538-7836.2012.04650.x.

Abstract

AIMS

This study aimed to (i) employ our newly designed model, the hypertensive-hypercholesterolemic hamster (HH), in order to find out whether a correlation exists between circulating microparticles (MPs), endothelial progenitor cells (EPCs) and their contribution to vascular dysfunction and (ii) to assess the effect of irbesartan treatment on HH animals (HHI).

METHODS AND RESULTS

The results showed that compared with the control (C) group, HH displayed: (i) a significant increase in plasma cholesterol and triglyceride concentration, and an augmentation of systolic and diastolic arterial blood pressure, and of heart rate; (ii) a marked elevation of MPs and a significant decrease in EPCs; (iii) structural modifications of the arterial wall correlated with altered protein expression of MMP2, MMP9, MMP12, TIMP1, TIMP2 and collagen type I and III; (iv) a considerably altered reactivity of the arterial wall closely correlated with MPs and EPC adherence; and (v) an inflammatory process characterized by augmented expression of P-Selectin, E-Selectin, von Willebrand factor, tissue factor, IL-6, MCP-1 and RANTES. Additionally, the experiments showed the potential of irbesartan to correct all altered parameters in HH and to mobilize EPCs by NO, chemokines and adhesion molecule-dependent mechanisms.

CONCLUSIONS

Hypertension associated with hypercholesterolemia is accompanied by structural modifications and expression of pro-inflammatory molecules by the vessel wall, the alteration of vascular tone, enhanced release of MPs and reduced EPCs; the ratio between the latter two may be considered as a marker of vascular dysfunction. Irbesartan, which exhibits a pharmacological control on the levels of MPs and EPCs, has the potential to restore homeostasis of the arterial wall.

摘要

目的

本研究旨在(i)利用我们新设计的模型,即高血压-高胆固醇血症仓鼠(HH),以确定循环微颗粒(MPs)、内皮祖细胞(EPCs)与其对血管功能障碍的贡献之间是否存在相关性,以及(ii)评估厄贝沙坦对 HH 动物(HHI)的治疗效果。

方法和结果

结果表明,与对照组(C)相比,HH 表现出:(i)血浆胆固醇和甘油三酯浓度显著升高,收缩压和舒张压以及心率升高;(ii)MPs 显著升高,EPCs 显著减少;(iii)动脉壁结构改变与 MMP2、MMP9、MMP12、TIMP1、TIMP2 和胶原 I 和 III 的蛋白表达改变相关;(iv)动脉壁反应性明显改变,与 MPs 和 EPC 黏附密切相关;(v)炎症过程表现为 P-选择素、E-选择素、血管性血友病因子、组织因子、IL-6、MCP-1 和 RANTES 表达增加。此外,实验表明厄贝沙坦具有纠正 HH 所有改变参数的潜力,并通过 NO、趋化因子和黏附分子依赖机制动员 EPCs。

结论

高血压伴高胆固醇血症会导致血管壁结构改变和促炎分子表达、血管张力改变、MPs 释放增加和 EPCs 减少;后两者之间的比值可作为血管功能障碍的标志物。厄贝沙坦对 MPs 和 EPCs 的水平具有药理学控制作用,具有恢复动脉壁内稳态的潜力。

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