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通过单分子测序揭示腺相关病毒载体的天然分子状态。

Native molecular state of adeno-associated viral vectors revealed by single-molecule sequencing.

机构信息

Helicos BioSciences , Cambridge, MA 02139, USA.

出版信息

Hum Gene Ther. 2012 Jan;23(1):46-55. doi: 10.1089/hum.2011.160. Epub 2011 Oct 4.

Abstract

The single-stranded genome of adeno-associated viral (AAV) vectors is one of the key factors leading to slow-rising but long-term transgene expression kinetics. Previous molecular studies have established what is now considered a textbook molecular model of AAV genomes with two copies of inverted tandem repeats at either end. In this study, we profiled hundreds of thousands of individual molecules of AAV vector DNA directly isolated from capsids, using single-molecule sequencing (SMS), which avoids any intermediary steps such as plasmid cloning. The sequence profile at 3' ends of both the regular and oversized vector did show the presence of an inverted terminal repeat (ITR), which provided direct confirmation that AAV vector packaging initiates from its 3' end. Furthermore, the vector 5'-terminus profile showed inconsistent termination for oversized vectors. Such incomplete vectors would not be expected to undergo canonical synthesis of the second strand of their genomic DNA and thus could function only via annealing of complementary strands of DNA. Furthermore, low levels of contaminating plasmid DNA were also detected. SMS may become a valuable tool during the development phase of vectors that are candidates for clinical use and for facilitating/accelerating studies on vector biology.

摘要

腺相关病毒(AAV)载体的单链基因组是导致慢起但长期转基因表达动力学的关键因素之一。以前的分子研究已经建立了现在被认为是 AAV 基因组的教科书分子模型,其两端各有两个拷贝的反向串联重复。在这项研究中,我们使用单分子测序(SMS)直接从衣壳中分离出数十万种 AAV 载体 DNA 分子,这种方法避免了质粒克隆等中间步骤。常规和超大载体 3' 末端的序列特征确实显示出存在反向末端重复(ITR),这直接证实了 AAV 载体包装从其 3' 末端开始。此外,载体 5' 末端特征显示超大载体的终止不一致。这种不完整的载体预计不会经历其基因组 DNA 第二链的典型合成,因此只能通过互补 DNA 链的退火来发挥功能。此外,还检测到低水平的污染质粒 DNA。SMS 可能成为候选临床应用的载体在开发阶段的有价值工具,并且有助于/加速载体生物学的研究。

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