腺相关病毒载体整合
Adeno-associated virus vector integration.
作者信息
Deyle David R, Russell David W
机构信息
University of Washington, Department of Biochemistry, Seattle, WA 98195, USA.
出版信息
Curr Opin Mol Ther. 2009 Aug;11(4):442-7.
Abstract
Adeno-associated virus (AAV) vectors efficiently transduce various cell types and can produce long-term expression of transgenes in vivo. Although AAV vector genomes can persist within cells as episomes, vector integration has been observed in various experimental settings, either at non-homologous sites where DNA damage may have occurred or by homologous recombination. In some cases, integration is essential for the therapeutic or experimental efficacy of AAV vectors. Recently, insertional mutagenesis resulting from the integration of AAV vectors was associated with tumorigenesis in mice, a consideration that may have relevance for certain clinical applications.
摘要
腺相关病毒(AAV)载体能高效转导多种细胞类型,并可在体内产生转基因的长期表达。尽管AAV载体基因组可作为附加体在细胞内持续存在,但在各种实验环境中均观察到载体整合现象,要么发生在可能出现DNA损伤的非同源位点,要么通过同源重组进行整合。在某些情况下,整合对于AAV载体的治疗或实验效果至关重要。最近,AAV载体整合导致的插入诱变与小鼠肿瘤发生有关,这一问题可能与某些临床应用相关。
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