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Rapid and highly efficient transduction by double-stranded adeno-associated virus vectors in vitro and in vivo.

机译:在体外和体内通过双链腺相关病毒载体进行快速高效的转导。

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Adeno-associated virus (AAV) is a promising gene vector based on a single-stranded (ss) DNA virus. Its transgene expression requires the conversion of ssDNA to double-stranded (ds) genome, a slow process responsible for the delayed transduction and occasional inefficiency. By mutating the inverted terminal repeat, we have made novel AAV vectors that predominantly package the self-complementary dsDNA genome. The dsAAV consistently demonstrated superior and accelerated transduction in vitro and in vivo. Dramatic increases in transgene expression were observed in most of the cell lines examined, including B16 melanoma and 3LL lung cancer that are difficult to be transduced by the conventional ssAAV vectors. Similar increases were also observed in vivo in a variety of tissues including muscle and liver. The dsAAV transduced a vast majority of the hepatocytes for more than 6 months, while the ssAAV transduced only a small fraction. In addition to circumventing the requirement for DNA synthesis, the dsAAV exhibited higher in vivo DNA stability and more effective circularization than the ssAAV, suggesting potential molecular mechanisms for the faster, stronger and prolonged transgene expression.Gene Therapy (2003) 10, 2105-2111. doi:10.1038/sj.gt.3302133
机译:腺相关病毒(AAV)是一种基于单链(ss)DNA病毒的有前途的基因载体。其转基因表达需要将ssDNA转化为双链(ds)基因组,这是一个缓慢的过程,导致延迟的转导和偶尔的低效率。通过突变反向末端重复序列,我们制备了新颖的AAV载体,这些载体主要包装了自身互补的dsDNA基因组。 dsAAV始终在体外和体内均表现出优异且加速的转导。在大多数检查的细胞系中观察到转基因表达的急剧增加,包括难以通过常规ssAAV载体转导的B16黑色素瘤和3LL肺癌。在体内包括肌肉和肝脏在内的各种组织中也观察到了类似的增加。 dsAAV转导了绝大多数肝细胞长达6个月以上,而ssAAV仅转导了一小部分。除了规避DNA合成的要求外,dsAAV还比ssAAV表现出更高的体内DNA稳定性和更有效的环化作用,提示了更快,更强和更长的转基因表达的潜在分子机制。基因治疗(2003)10,2105-2111 。 doi:10.1038 / sj.gt.3302133

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