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The effect of controlled expression of VEGF by transduced myoblasts in a cardiac patch on vascularization in a mouse model of myocardial infarction

机译:VEGF对血管蛋白在心肌梗死小鼠模型中血管蛋白在心脏贴片中的转导肌细胞的影响

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摘要

Key requirements for cardiac tissue engineering include the maintenance of cell viability and function and the establishment of a perfusable vascular network in millimeters thick and compact cardiac constructs upon implantation. We investigated if these requirements can be met by providing an intrinsic vascularization stimulus (via sustained action of VEGF secreted at a controlled rate by transduced myoblasts) to a cardiac patch engineered under conditions of effective oxygen supply (via medium flow through channeled elastomeric scaffolds seeded with neonatal cardiomyocytes). We demonstrate that this combined approach resulted in increased viability, vascularization and functionality of the cardiac patch. After implantation in a mouse model of myocardial infarction, VEGF-expressing patches displayed significantly improved engraftment, survival and differentiation of cardiomyocytes, leading to greatly enhanced contractility as compared to controls not expressing VEGF. Controlled VEGF expression also mediated the formation of mature vascular networks, both within the engineered patches and in the underlying ischemic myocardium. We propose that this combined cell-biomaterial approach can be a promising strategy to engineer cardiac patches with intrinsic and extrinsic vascularization potential.
机译:心脏组织工程的关键要求包括维持细胞活力和功能,以及在植入后以毫米厚且紧凑的心脏结构建立可灌注的血管网络。我们研究了通过向有效氧供应条件下改造的心脏贴片提供固有的血管生成刺激(通过以受控速率通过转导的成肌细胞分泌的VEGF的持续作用)来满足这些要求(通过介质流经植入有新生儿心肌细胞)。我们证明,这种组合的方法导致增加了活力,血管生成和功能的心脏补丁。植入心肌梗塞小鼠模型后,表达VEGF的贴片显示出显着改善的心肌细胞植入,存活和分化,与不表达VEGF的对照相比,可收缩性大大增强。受控的VEGF表达也介导了成熟的血管网络的形成,无论是在工程补丁中还是在潜在的缺血性心肌中。我们建议这种组合的细胞-生物材料方法可能是一种有前途的策略,以设计具有内在和外在血管生成潜力的心脏补丁。

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