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Brain Angiogenesis Induced by Nonviral Gene Therapy with Potential Therapeutic Benefits for Central Nervous System Diseases

机译:非血流基因治疗脑血管生成,具有中枢神经系统疾病的潜在治疗益处

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摘要

Gene therapy employing nanocarriers represents a promising strategy to treat central nervous system (CNS) diseases, where brain microvasculature is frequently compromised. Vascular endothelial growth factor (VEGF) is a key angiogenic molecule; however, its in vivo administration to the CNS by nonviral gene therapy has not been conducted. Hence, we prepared and physicochemically characterized four cationic niosome formulations (1-4), which were combined with pVEGF-GFP to explore their capacity to transfer the VEGF gene to CNS cells and achieve angiogenesis in the brain. Experiments in primary neuronal cells showed successful and safe transfection with niosome 4, producing double levels of biologically active VEGF in comparison to the rest of the formulations. Intracortical administration of niosome 4 based nioplexes in mouse brain validated the ability of this nonviral vector to deliver the VEGF gene to CNS cells, inducing brain angiogenesis and emerging as a promising therapeutic approach for the treatment of CNS diseases.
机译:使用纳米载波的基因治疗代表了治疗中枢神经系统(CNS)疾病的有希望的策略,其中脑微血管经常受到损害。血管内皮生长因子(VEGF)是关键的血管生成分子;然而,它在通过非血流基因治疗对CNS的体内给药。因此,我们制备和理化化学表征了四种阳离子定位制剂(1-4),其与PVEGF-GFP组合以探讨其将VEGF基因转移到CNS细胞的能力并在大脑中实现血管生成。原发性神经元细胞的实验表明,与术语4的成功和安全转染,与其他配方相比,产生双层生物活性VEGF。在小鼠脑中术基术治疗术的术基嗜酸性4的核施用验证了该非血管载体将VEGF基因递送到CNS细胞的能力,诱导脑血管生成和新兴作为治疗CNS疾病的有希望的治疗方法。

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