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首页> 外文期刊>Journal of atherosclerosis and thrombosis. >Angiogenesis Inhibitor, Endostar, Prevents Vasa Vasorum Neovascularization in a Swine Atherosclerosis Model
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Angiogenesis Inhibitor, Endostar, Prevents Vasa Vasorum Neovascularization in a Swine Atherosclerosis Model

机译:血管生成抑制剂Endostar在猪动脉粥样硬化模型中预防Vasa Vasorum新生血管形成

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Aim : Vasa vasorum neovascularization is a key feature of atherosclerosis (AS) and is strongly associated with inflammatory infiltration, lipid deposition, intraplaque hemorrhage, and hemosiderin deposit. Here we investigate the effects of Endostar, a strong anti-angiogenic drug, on vasa vasorum neovascularization in the experimental porcine model of early AS. Methods : Eighteen adult male Ba-Ma mini pigs were randomized into three groups, with six animals in each group. The pigs in the normal (N) group were fed a normal diet for 18 weeks, without balloon injury surgery. The animals in the atherosclerotic (AS) control and AS+Endostar groups were fed a hypercholesterolemic diet for 12 weeks after balloon injury surgery; they received either saline or Endostar for an additional six weeks, while continuing the hypercholesterolemic diet. The atherosclerotic abdominal aorta and levels of serum lipids, TNF-alpha, IL-6, and hs-CRP were analyzed at 18 weeks. Results : The AS group had a significantly higher body weight and serum lipid concentration levels than the N group ( p <0.05), confirming the success of the hypercholesterolemic diet. However, no statistical differences were noted between the AS and AS+Endostar groups. Histopathology results revealed that vasa vasorum density and intima–media thickness (IMT) had also increased in the AS group compared with those in the N group ( p <0.05). The Endostar treatment significantly alleviated AS with decreased vasa vasorum density and IMT (AS vs. AS+Endostar, p <0.05). Western blot analysis indicated that the expression of VEGF, β-catenin, and TNF-alpha in the atherosclerotic abdominal aorta was considerably reduced by the Endostar treatment. In addition, immunohistochemistry results showed that the angiogenesis markers VEGF and β-catenin were predominately localized in endothelial cells of the adventitial vasa vasorum. The levels of the serum inflammatory markers TNF-alpha, hs-CRP, and IL-6 were markedly higher in the AS group than in the N group ( p <0.05) but showed no marked difference during the Endostar treatment, suggesting that the local inhibition of angiogenesis was not accompanied by a change in serum inflammatory markers and that the inhibitive effect of Endostar on local TNF-alpha expression could be because of the prevention of vasa vasorum neovascularization. Conclusions : Our results demonstrated that the Endostar treatment inhibited vasa vasorum neovascularization and AS progression in the experimental porcine model of early AS, supporting the role of vasa vasorum neovascularization in the development of AS and the therapeutic potential of anti-angiogenesis intervention in AS.
机译:目的:脉管血管新生血管形成是动脉粥样硬化(AS)的关键特征,与炎症浸润,脂质沉积,斑块内出血和铁血黄素沉积密切相关。在这里,我们研究了在早期AS的实验性猪模型中,抗血管生成药物Endostar对血管新生血管新生的作用。方法:将十八头成年雄性Ba-Ma小型猪随机分为三组,每组六只。正常(N)组的猪在不进行球囊损伤手术的情况下接受了18周的正常饮食。球囊损伤手术后12周,对动脉粥样硬化(AS)对照组和AS + Endostar组的动物进行高胆固醇饮食。他们在继续高胆固醇饮食的同时又接受了盐水或Endostar治疗六周。在18周时分析了腹主动脉粥样硬化和血清脂质,TNF-α,IL-6和hs-CRP的水平。结果:AS组的体重和血脂水平明显高于N组(p <0.05),证实了高胆固醇饮食的成功。但是,AS组和AS + Endostar组之间没有统计学差异。组织病理学结果显示,与N组相比,AS组的脉管血管密度和内膜中层厚度(IMT)也增加了(p <0.05)。 Endostar治疗可显着缓解AS,同时降低血管血管密度和IMT(AS vs. AS + ​​Endostar,p <0.05)。 Western印迹分析表明,Endostar治疗可显着降低动脉粥样硬化腹主动脉中VEGF,β-catenin和TNF-α的表达。另外,免疫组织化学结果表明,血管生成标记物VEGF和β-连环蛋白主要定位于外膜脉管的内皮细胞中。 AS组血清炎症标志物TNF-α,hs-CRP和IL-6的水平明显高于N组(p <0.05),但在Endostar治疗期间无明显差异,提示局部抑制血管新生并不伴随血清炎性标志物的改变,Endostar对局部TNF-α表达的抑制作用可能是由于预防了血管新生血管的形成。结论:我们的结果表明,Endostar治疗可抑制早期AS实验猪模型中血管新生血管的形成和AS的进展,支持血管新生血管在AS的发展中的作用以及抗血管生成干预AS的治疗潜力。

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