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首页> 外文期刊>Surgery >Antisense oligonucleotides to c-fos and c-jun inhibit intimal thickening in a rat vein graft model.
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Antisense oligonucleotides to c-fos and c-jun inhibit intimal thickening in a rat vein graft model.

机译:c-fos和c-jun的反义寡核苷酸可抑制大鼠静脉移植模型的内膜增厚。

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摘要

BACKGROUND: C-fos and c-jun are 2 immediate early genes that have been implicated in the stimulation of vascular smooth muscle cell proliferation and migration. In previous experiments in our laboratory with a rat vein graft model a 2- to 3-fold increase of messenger RNA of c-fos and c-jun were noted 1 hour after vein graft perfusion. Because c-fos and c-jun are up-regulated after the perfusion of vein grafts, the purpose of this study was to delineate the temporal expression of c-fos and c-jun protein and to study the effect of antisense oligonucleotides (ASO) to c-fos and c-jun on intimal thickening observed in this model. METHODS: Sprague-Dawley rats underwent bilateral interposition femoral artery grafts with use of the superficial epigastric vein, which was harvested from 15 minutes up to 2 weeks and analyzed by Western blot for Fos and Jun protein. Additional rats underwent bypasses and at the time of the procedure 1 graft was treated with a pluronic gel containing an ASO to c-fos, c-jun, or sense and the contralateral side was treated with pluronic gel only. The vein grafts were harvested 2 weeks after the procedure and perfusion fixed. After longitudinal sectioning, the intimal and total wall thicknesses were measured in the perianastamotic and midgraft regions by a morphometric digitizing microscope and the statistics were analyzed by a paired Student's t test. RESULTS: Protein analysis by Western blot showed that c-fos levels rose quickly within 2 hours and leveled at 6 hours 40-fold above basal levels after vein graft perfusion. Similarly, c-jun levels rose 10-fold above basal levels after 15 minutes and peaked at 2 hours 120-fold above basal levels. The treatment of the vein grafts with these ASOs resulted in a reduction of about 30% in the thickness of the intimal layer and the total wall thickness in both the perianastomotic and the midgraft regions, which was statistically significant different from control veins. CONCLUSION: These results indicate a possible therapeutic role for ASO to immediate early genes in the treatment of vein graft intimal hyperplasia.
机译:背景:C-fos和c-jun是2个立即早期基因,与刺激血管平滑肌细胞增殖和迁移有关。在我们实验室中使用大鼠静脉移植物模型进行的先前实验中,在静脉移植物灌注1小时后,注意到c-fos和c-jun的信使RNA增加了2到3倍。由于c-fos和c-jun在静脉移植物灌注后被上调,因此本研究的目的是描绘c-fos和c-jun蛋白的时间表达并研究反义寡核苷酸(ASO)的作用在此模型中观察到c-fos和c-jun对内膜增厚的影响。方法:Sprague-Dawley大鼠使用上腹部浅表静脉进行双侧介入性股动脉移植,从15分钟到2周的时间收集并通过Western印迹分析Fos和Jun蛋白。额外的大鼠进行旁路手术,在步骤1时,将移植物用含ASO的c-fos,c-jun或有义ASO的普朗尼克凝胶处理,而对侧仅用普朗尼克凝胶处理。手术后2周收集静脉移植物,并固定灌注。纵向切片后,通过形态计量数字显微镜在经肛门和中部移植物区域测量内膜厚度和总壁厚度,并通过配对的t检验对统计数据进行分析。结果:蛋白免疫印迹分析表明,静脉移植后c-fos水平在2小时内迅速升高,并在6小时时升高,比基础水平高40倍。同样,c-jun水平在15分钟后比基础水平上升了10倍,并在2小时达到了比基础水平高120倍的峰值。用这些ASO对静脉移植物进行处理后,经肛门口和中段移植区的内膜层厚度和总壁厚均减少了约30%,这在统计学上与对照静脉有显着差异。结论:这些结果表明,ASO对早期早期基因在静脉移植物内膜增生的治疗中可能具有治疗作用。

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