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首页> 外文期刊>The journal of gene medicine >Evaluation of angiogenesis and side effects in ischemic rabbit hindlimbs after intramuscular injection of adenoviral vectors encoding VEGF and LacZ
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Evaluation of angiogenesis and side effects in ischemic rabbit hindlimbs after intramuscular injection of adenoviral vectors encoding VEGF and LacZ

机译:肌内注射编码VEGF和LacZ的腺病毒载体后对缺血兔后肢血管生成和副作用的评估

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摘要

Background Recent studies have suggested the therapeutic potential of vascular endothelial growth factor (VEGF) gene therapy in ischemic skeletal muscle. However, only limited information is available about the effect of VEGF gene therapy in different regions of ischemic limbs, effects of control adenoviruses, and biodistribution of the transgenes after intramuscular (i.m.) administration. Here we studied angiogenesis and side effects of adenovirusmediated VEGF and β-galactosidase (LacZ) gene transfers in ischemic rabbit hindlimbs. Methods and results Ten days after induction of ischemia, rabbits were treated with i.m. injections of saline, LacZ adenovirus (AdLacZ; 2 * 10~(10) pfu) or adenovirus encoding mouse VEGF_(164) (AdVEGF; 2 * 10~(10) pfu). In rabbits treated with AdVEGF an increase in serum VEGF_(164) levels was detected by ELISA three and seven days after the gene transfer. 30 days after the gene transfer a positive effect on capillary density was observed in the thigh region both in rabbits treated with AdVEGF and AdLacZ compared with animals that received saline. On the other hand, AdVEGF and AdLacZ gene transfers had no effect on the capillary density in the calf region on day 30. A positive correlation between the capillary density and the number of collateral arteries was observed in the thigh. Hindlimb and testis edema and excess nonphysiological growth of capillaries were detected as adverse effects of the AdVEGF gene therapy. Biodistribution analysis showed that the transgene was present not only in the target muscle, but also in ectopic tissues seven days after i.m. gene transfer. Conclusions The results suggest that a high dose of adenoviral vector encoding either AdVEGF or AdLacZ induces angiogenesis in the rabbit hindlimb ischemia model; i.m. injection of adenovirus leads to the transfection of ectopic organs; and AdVEGF gene transfer induces edema in ischemic skeletal muscle.
机译:背景技术最近的研究表明,血管内皮生长因子(VEGF)基因治疗在缺血性骨骼肌中具有治疗潜力。但是,关于血管内(i.m.)施用后VEGF基因治疗在缺血肢体不同区域的作用,对照腺病毒的作用以及转基因的生物分布,只有有限的信息。在这里,我们研究了缺血兔后肢中腺病毒介导的VEGF和β-半乳糖苷酶(LacZ)基因转移的血管生成和副作用。方法和结果诱导缺血10天后,用i.m处理兔。注射盐水,LacZ腺病毒(AdLacZ; 2 * 10〜(10)pfu)或编码小鼠VEGF_(164)(AdVEGF; 2 * 10〜(10)pfu)的腺病毒。基因转移后三天和第七天,用AdVEGF处理的兔的ELISA检测到血清VEGF_(164)水平升高。基因转移后30天,与接受生理盐水处理的动物相比,经AdVEGF和AdLacZ处理的兔子在大腿区域均观察到了对毛细血管密度的积极影响。另一方面,在第30天,AdVEGF和AdLacZ基因转移对小腿区域的毛细血管密度没有影响。在大腿中,毛细血管密度与侧支动脉数量之间呈正相关。检测到后肢和睾丸水肿以及毛细血管过度非生理生长是AdVEGF基因治疗的不良反应。生物分布分析表明,转基因不仅存在于目标肌肉中,而且在i.m后7天也存在于异位组织中。基因转移。结论结果表明,高剂量编码AdVEGF或AdLacZ的腺病毒载体在兔后肢缺血模型中诱导血管生成。我注射腺病毒导致异位器官的转染; AdVEGF基因转移可引起缺血性骨骼肌水肿。

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