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Dual functionalized liposome-mediated gene delivery across triple co-culture blood brain barrier model and specific in vivo neuronal transfection

机译:跨三重共培养血脑屏障模型和特定体内神经元转染的双重功能化脂质体介导的基因传递

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摘要

Gene therapy has become a promising approach for neurodegenerative disease treatment, however there is an urgent need to develop an efficient gene carrier to transport gene across the blood brain barrier (BBB). In this study, we strategically designed dual functionalized liposomes for efficient neuronal transfection by combining transferrin (Tf) receptor targeting and enhanced cell penetration utilizing penetratin (Pen). A triple cell co-culture model of BBB confirmed the ability of the liposomes to cross the barrier layer and transfect primary neuronal cells. In vivo quantification of PenTf-liposomes demonstrated expressive accumulation in the brain (12%), without any detectable cellular damage or morphological change. The efficacy of these nanoparticles containing plasmid β-galactosidase in modulating transfection was assessed by β-galactosidase expression in vivo. As a consequence of accumulation in the brain, PenTf-liposomes significantly induced gene expression in mice. Immunofluorescence studies of brain sections of mice after tail vein injection of liposomes encapsulating pDNA encoding GFP (pGFP) illustrate the superior ability of dual- functionalized liposomes to accumulate in the brain and transfect neurons. Taken together, the multifunctional liposomes provide an excellent gene delivery platform for neurodegenerative diseases.
机译:基因疗法已成为治疗神经退行性疾病的一种有前途的方法,但是迫切需要开发一种有效的基因载体,以通过血脑屏障(BBB)转运基因。在这项研究中,我们通过结合转铁蛋白(Tf)受体靶向和利用渗透素(Pen)增强的细胞渗透性,策略性地设计了用于高效神经元转染的双重功能化脂质体。 BBB的三细胞共培养模型证实了脂质体穿过屏障层并转染原代神经元细胞的能力。 PenTf-脂质体的体内定量显示在脑中有表达积聚(12%),而没有任何可检测到的细胞损伤或形态变化。通过体内β-半乳糖苷酶表达来评估这些包含质粒β-半乳糖苷酶的纳米颗粒在调节转染中的功效。由于在大脑中积累,PenTf-脂质体显着诱导了小鼠中的基因表达。尾静脉注射包裹编码GFP(pGFP)的pDNA的脂质体后,对小鼠大脑切片的免疫荧光研究表明,双功能脂质体在大脑中积聚和转染神经元具有卓越的能力。综上所述,多功能脂质体为神经退行性疾病提供了极好的基因传递平台。

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