首页> 美国卫生研究院文献>Stem Cells International >Comparative AAV-eGFP Transgene Expression Using Vector Serotypes 1–9 7m8 and 8b in Human Pluripotent Stem Cells RPEs and Human and Rat Cortical Neurons
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Comparative AAV-eGFP Transgene Expression Using Vector Serotypes 1–9 7m8 and 8b in Human Pluripotent Stem Cells RPEs and Human and Rat Cortical Neurons

机译:使用人类多能干细胞RPE和人类和大鼠皮质神经元的血清型1–9、7m8和8b比较AAV-eGFP转基因表达

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摘要

Recombinant adeno-associated virus (rAAV), produced from a nonpathogenic parvovirus, has become an increasing popular vector for gene therapy applications in human clinical trials. However, transduction and transgene expression of rAAVs can differ across in vitro and ex vivo cellular transduction strategies. This study compared 11 rAAV serotypes, carrying one reporter transgene cassette containing a cytomegalovirus immediate-early enhancer (eCMV) and chicken beta actin (CBA) promoter driving the expression of an enhanced green-fluorescent protein (eGFP) gene, which was transduced into four different cell types: human iPSC, iPSC-derived RPE, iPSC-derived cortical, and dissociated embryonic day 18 rat cortical neurons. Each cell type was exposed to three multiplicity of infections (MOI: 1E4, 1E5, and 1E6 vg/cell). After 24, 48, 72, and 96 h posttransduction, GFP-expressing cells were examined and compared across dosage, time, and cell type. Retinal pigmented epithelium showed highest AAV-eGFP expression and iPSC cortical the lowest. At an MOI of 1E6 vg/cell, all serotypes show measurable levels of AAV-eGFP expression; moreover, AAV7m8 and AAV6 perform best across MOI and cell type. We conclude that serotype tropism is not only capsid dependent but also cell type plays a significant role in transgene expression dynamics.
机译:由非致病性细小病毒产生的重组腺伴随病毒(rAAV)已成为在人类临床试验中用于基因治疗的越来越流行的载体。但是,rAAVs的转导和转基因表达可能在体外和离体细胞转导策略中有所不同。这项研究比较了11种rAAV血清型,携带一个报告基因转基因盒,其中包含巨细胞病毒立即早期增强子(eCMV)和鸡β肌动蛋白(CBA)启动子,驱动表达增强的绿色荧光蛋白(eGFP)基因,该基因被转导为四个不同的细胞类型:人类iPSC,iPSC衍生的RPE,iPSC衍生的皮质,以及离体的第18天胚胎大鼠皮质神经元。每种细胞类型都暴露于三种感染(MOI:1E4、1E5和1E6 + vg /细胞)。转导后24、48、72和96h,检查表达GFP的细胞,并比较剂量,时间和细胞类型。视网膜色素上皮显示最高的AAV-eGFP表达,而iPSC皮质的最低。在MOE为1E6 vg /细胞时,所有血清型均显示可测量的AAV-eGFP表达水平;此外,AAV7m8和AAV6在MOI和细胞类型方面表现最佳。我们得出结论,血清型嗜性不仅取决于衣壳,而且细胞类型在转基因表达动力学中也起着重要作用。

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