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单极性DNA基因组的腺相关病毒能够在体内进行转导。

Adeno-associated virus of a single-polarity DNA genome is capable of transduction in vivo.

作者信息

Zhou Xiaohuai, Zeng Xinghua, Fan Zhenghong, Li Chengwen, McCown Thomas, Samulski R Jude, Xiao Xiao

机构信息

Gene Therapy Center, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina 27599, USA.

出版信息

Mol Ther. 2008 Mar;16(3):494-9. doi: 10.1038/sj.mt.6300397. Epub 2008 Jan 8.

Abstract

The adeno-associated virus (AAV) is a promising vector for gene therapy. Further improvement of the virus for clinical application depends on better understanding of the molecular structure and fate of the vector genome. AAV vectors with wild-type inverted terminal repeats package either the plus- or the minus-strand DNA genomes with equal frequency. By creating a series of deletions within the, we have developed a genetic approach that can generate an AAV vector that packages its single-stranded DNA genome predominantly in a single polarity (99.4%). This novel reagent efficiently transduced muscle, brain and liver in whole animals. The transduction efficiencies were similar to those of the control mixed-polarity vectors. Our results showed that reannealing of plus- and minus-strand DNA was not required for AAV-mediated transduction in vivo, supporting the hypothesis that second-strand DNA synthesis is a primary pathway in converting the single-stranded AAV genome into double-stranded forms. The availability of the single-polarity AAV vector would aid further studies on the mechanism of AAV transduction as well as the application of AAV vector for gene replacement therapy.

摘要

腺相关病毒(AAV)是一种很有前景的基因治疗载体。要进一步改进该病毒用于临床,取决于对载体基因组的分子结构和命运有更深入的了解。具有野生型反向末端重复序列的AAV载体以相等频率包装正链或负链DNA基因组。通过在其中创建一系列缺失,我们开发了一种遗传方法,该方法可以产生一种AAV载体,其单链DNA基因组主要以单一极性(99.4%)进行包装。这种新型试剂能有效地在整体动物中转导肌肉、大脑和肝脏。转导效率与对照混合极性载体相似。我们的结果表明,在体内AAV介导的转导不需要正链和负链DNA的重新退火,这支持了以下假设:第二链DNA合成是将单链AAV基因组转化为双链形式的主要途径。单极性AAV载体的可用性将有助于进一步研究AAV转导机制以及AAV载体在基因替代治疗中的应用。

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