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使用含有柯萨奇病毒和腺病毒受体cDNA的重组腺病毒载体将基因高效重复递送至骨骼肌。

Efficient repetitive gene delivery to skeletal muscle using recombinant adenovirus vector containing the Coxsackievirus and adenovirus receptor cDNA.

作者信息

Kimura E, Maeda Y, Arima T, Nishida Y, Yamashita S, Hara A, Uyama E, Mita S, Uchino M

机构信息

Department of Neurology, Kumamoto University School of Medicine, 1-1-1 Honjo, Kumamoto 860-0811 Japan.

出版信息

Gene Ther. 2001 Jan;8(1):20-7. doi: 10.1038/sj.gt.3301359.

Abstract

To improve adenovirus-mediated gene delivery to skeletal muscle, we have used a recombinant adenovirus vector encoding the human Coxsackievirus and adenovirus receptor (hCAR). Because CAR is expressed at a lower level in rodent myoblasts and muscle fibers than in other tissues, we expected that elevated expression of CAR in skeletal muscle would improve the efficacy of adenovirus-mediated gene transfer. Since the mouse myoblasts, C2C12 cells, showed low sensitivity to infection by recombinant adenovirus 5, we initially infected these cells at a high multiplicity of infection (MOI) of 250 with the recombinant adenovirus containing hCAR cDNA and LacZ gene. Subsequent infection by recombinant adenovirus containing the marker gene, green fluorescence protein, became efficient even at a low MOI of 25. Thus, elevated hCAR expression in mouse muscle fibers made a second virus inoculation at low doses possible. We also demonstrated that the elevated hCAR expression did not influence muscle membrane integrity. Our results suggest that co-expression of CAR and a therapeutic gene by adenovirus vector constitutes a novel strategy to advance gene therapy for hereditary muscle diseases.

摘要

为了提高腺病毒介导的基因向骨骼肌的递送效率,我们使用了一种编码人柯萨奇病毒和腺病毒受体(hCAR)的重组腺病毒载体。由于CAR在啮齿动物成肌细胞和肌纤维中的表达水平低于其他组织,我们预计提高骨骼肌中CAR的表达会提高腺病毒介导的基因转移效率。由于小鼠成肌细胞C2C12细胞对重组腺病毒5感染的敏感性较低,我们最初以250的高感染复数(MOI)用含有hCAR cDNA和LacZ基因的重组腺病毒感染这些细胞。随后用含有标记基因绿色荧光蛋白的重组腺病毒进行感染,即使在25的低MOI下也变得高效。因此,小鼠肌纤维中hCAR表达的升高使得低剂量的第二次病毒接种成为可能。我们还证明,hCAR表达的升高不会影响肌膜完整性。我们的结果表明,腺病毒载体共表达CAR和治疗性基因构成了一种推进遗传性肌肉疾病基因治疗的新策略。

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