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Effects of local gene transfer of VEGF on neointima formation after balloon injury in hypercholesterolemic rabbits

机译:VEGF局部基因转移对高胆固醇血症兔球囊损伤后新内膜形成的影响

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摘要

Enhancement of the generation of nitric oxide (NO) and vascular endothelial growth factor (VEGF) are suggested to prevent restenosis after angioplasty. Accordingly, we tested whether the local delivery of l-arginine (l-Arg), a substrate for NO generation and the VEGF gene, alone or in combination, can influence neointima formation in hypercholesterolemic rabbits. Balloon injury of the iliac arteries was performed in 24 New Zealand White rabbits fed a 1% cholesterol diet for 3 weeks followed by a local infusion of: (1) pSG5VEGF165 plasmid alone (1000 μg); (2) pSG5VEGF165 (1000 μg) with l-Arg (800 mg); (3) l-Arg (800 mg) alone; and (4) l-Arg (800 mg) with naked pSVβ-gal plasmid (1000 μg). The animals were kept on the hypercholesterolemic diets for a further 28 days, when vessels were taken for morphometric analysis and immunocytochemistry. Endogenous rabbit VEGF concentration in the plasma increased significantly at 7 days after injury (17.06 ± 1.57 vs 23.01 ± 1.9 pg/ml; p < 0.02) and remained elevated for up to 28 days (28.46 ± 5.24; p < 0.01). Injured arteries exhibited strong immunocytochemical staining for rabbit VEGF. Rabbits that received a VEGF gene transfer revealed more prominent neointima formation, whereas treatment with l-Arg was associated with significantly less intimal thickness (p < 0.05). Local transfer of the VEGF gene does not inhibit neointima formation in hypercholesterolemic rabbits. Our results suggest that VEGF gene therapy applied locally in atherosclerotic arteries may not be beneficial.
机译:建议增加一氧化氮(NO)和血管内皮生长因子(VEGF)的生成,以防止血管成形术后的再狭窄。因此,我们测试了单独或组合使用l-精氨酸(l-Arg),NO生成的底物和VEGF基因的局部递送是否可以影响高胆固醇血症兔的新内膜形成。喂食1%胆固醇的3只新西兰白兔进行了3周的the动脉球囊损伤,然后局部输注:(1)仅pSG5VEGF165质粒(1000μg); (2)pSG5VEGF165(1000μg)与l-Arg(800 mg); (3)仅l-Arg(800毫克); (4)带有裸pSVβ-gal质粒(1000μg)的1-Arg(800mg)。当取血管进行形态分析和免疫细胞化学分析时,将这些动物在高胆固醇饮食中再饲养28天。损伤后第7天血浆中内源性兔VEGF浓度显着增加(17.06±1.57 vs 23.01±1.9 pg / ml; p <0.02),并保持升高长达28天(28.46±5.24; p <0.01)。受伤的动脉对兔VEGF表现出较强的免疫细胞化学染色。接受VEGF基因转移的兔子显示出更多的新内膜形成,而用l-Arg进行治疗的内膜厚度则显着减少(p <0.05)。 VEGF基因的局部转移不会抑制高胆固醇血症兔的新内膜形成。我们的结果表明,在动脉粥样硬化动脉中局部应用VEGF基因治疗可能不是有益的。

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