阿托伐他汀治疗后颈动脉损伤大鼠新生内膜增生的抑制可能主要与生存素和Fas表达下调有关。

Inhibition of neointimal hyperplasia in rats treated with atorvastatin after carotid artery injury may be mainly associated with down-regulation of survivin and Fas expression.

作者信息

Xu Yiguan, Zhou Shenghua, Fang Zhenfei, Li Xuping, Huang Dekui, Liu Qiliang, Zheng Chunhua

机构信息

Department of Cardiology, Shanghai Putuo District People's Hospital of Anwei Medical University , Shanghai , People's Republic of China .

出版信息

Pharm Biol. 2014 Sep;52(9):1196-203. doi: 10.3109/13880209.2014.884605.

DOI:10.3109/13880209.2014.884605

PMID:25116077

Abstract

CONTEXT

Atorvastatin is a member of the drug class known as statins, which is used for lowering blood cholesterol.

OBJECTIVE

The present study investigates the effect and mechanism of atorvastatin on neointimal hyperplasia after carotid artery injury (CAI) of rat.

MATERIALS AND METHODS

Fifty male rats were randomly divided into four groups: control group, sham-operated group, model group, and atorvastatin treatment group. The treatment group was fed with atorvastatin (10 mg/kg) with gastro-gavage at 5 p.m. every day for 28 d after surgery. The control group, model group, and sham-operated group were fed with the same volume of distilled water instead. The proliferations of intimal and medial layers were evaluated by hematoxylin & eosin (H&E) staining. The apoptosis of vascular smooth muscle cells (VSMCs) was determined by terminal deoxynucleotidyl transferased UTP nick end labeling (TUNEL) staining. Plasma concentrations of survivin and sFas were detected by enzyme-linked immunosorbent assay (ELISA).

RESULTS

Atorvastatin reduced neointimal formation and increased apoptosis of VSMCs in neointima. VSMCs apoptosis emerged at 3 d (8.42 ± 0.449 μm) and the intimal proliferation peaked by the end of 14 d (41.58 ± 1.64 μm). The plasma levels of survivin and sFas were gradually increased with the neointimal hyperplasia and increasingly decreased after atorvastatin treatment. The plasma levels of survivin and sFas in rats were elevated at 3 d (464.80 ± 105.27 pg/ml and 3256.00 ± 478.20 pg/ml, respectively), reached the peak of survivin at 14 d (1089.20 ± 232.32 pg/ml) and sFas at 7 d (4362.00 ± 639.92 pg/ml) and decreased at 28 d (562.00 ± 90.11 pg/ml and 2148.00 ± 257.14 pg/ml, respectively) in the model group. Compared with the model group, the atorvastatin treatment group has significantly less neointimal hyperplasia and more apoptosis of VSMCs.

CONCLUSIONS

Atorvastatin can inhibit neointimal hyperplasia and promote SMCs apoptosis in neointimal layers, which may be mainly associated with down-regulation of survivin and Fas expression after CAI of rat.

摘要

背景

阿托伐他汀是一类被称为他汀类药物的成员，用于降低血液胆固醇。

目的

本研究探讨阿托伐他汀对大鼠颈动脉损伤（CAI）后新生内膜增生的影响及机制。

材料与方法

50只雄性大鼠随机分为四组：对照组、假手术组、模型组和阿托伐他汀治疗组。治疗组在术后每天下午5点经胃管给予阿托伐他汀（10mg/kg），持续28天。对照组、模型组和假手术组给予相同体积的蒸馏水。通过苏木精和伊红（H&E）染色评估内膜和中膜层的增殖。通过末端脱氧核苷酸转移酶介导的dUTP缺口末端标记（TUNEL）染色测定血管平滑肌细胞（VSMC）的凋亡。采用酶联免疫吸附测定（ELISA）检测血浆中生存素和sFas的浓度。

结果

阿托伐他汀减少了新生内膜形成并增加了新生内膜中VSMC的凋亡。VSMC凋亡在3天时出现（8.42±0.449μm），内膜增殖在14天时达到峰值（41.58±1.64μm）。随着新生内膜增生，血浆中生存素和sFas水平逐渐升高，阿托伐他汀治疗后逐渐降低。模型组大鼠血浆中生存素和sFas水平在3天时升高（分别为464.80±105.27pg/ml和3256.00±478.20pg/ml），生存素在14天时达到峰值（1089.20±232.32pg/ml），sFas在7天时达到峰值（4362.00±639.92pg/ml），在28天时降低（分别为562.00±90.11pg/ml和2148.00±257.14pg/ml）。与模型组相比，阿托伐他汀治疗组新生内膜增生明显减少，VSMC凋亡增多。