In vitro evaluation of a double-stranded self-complementary adeno-associated virus type2 vector in bone marrow stromal cells for bone healing.

Farhang Alaee, Osamu Sugiyama, Mandeep S Virk, Ying Tang, Bing Wang, Jay R Lieberman
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引用次数: 6

Abstract

Background: Both adenoviral and lentiviral vectors have been successfully used to induce bone repair by over-expression of human bone morphogenetic protein 2 (BMP-2) in primary rat bone marrow stromal cells in pre-clinical models of ex vivo regional gene therapy. Despite being a very efficient means of gene delivery, there are potential safety concerns that may limit the adaptation of these viral vectors for clinical use in humans. Recombinant adeno-associated viral (rAAV) vector is a promising viral vector without known pathogenicity in humans and has the potential to be an effective gene delivery vehicle to enhance bone repair. In this study, we investigated gene transfer in rat and human bone marrow stromal cells in order to evaluate the effectiveness of the self-complementary AAV vector (scAAV) system, which has higher efficiency than the single-stranded AAV vector (ssAAV) due to its unique viral genome that bypasses the rate-limiting conversion step necessary in ssAAV.

Methods: Self-complementaryAAV2 encoding GFP and BMP-2 (scAAV2-GFP and scAAV2-BMP-2) were used to transduce human and rat bone marrow stromal cells in vitro, and subsequently the levels of GFP and BMP-2 expression were assessed 48 hours after treatment. In parallel experiments, adenoviral and lentiviral vector mediated over-expression of GFP and BMP-2 were used for comparison.

Results: Our results demonstrate that the scAAV2 is not capable of inducing significant transgene expression in human and rat bone marrow stromal cells, which may be associated with its unique tropism.

Conclusions: In developing ex vivo gene therapy regimens, the ability of a vector to induce the appropriate level of transgene expression needs to be evaluated for each cell type and vector used.

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骨髓基质细胞中双链自互补腺相关病毒2型载体对骨愈合的体外评价。
背景:在离体区域基因治疗的临床前模型中,腺病毒和慢病毒载体已经成功地通过在原代大鼠骨髓基质细胞中过表达人骨形态发生蛋白2 (BMP-2)来诱导骨修复。尽管是一种非常有效的基因传递手段,但存在潜在的安全问题,可能会限制这些病毒载体在人类临床应用中的适应性。重组腺相关病毒(rAAV)载体是一种很有前途的病毒载体,在人类中没有已知的致病性,有可能成为一种有效的基因传递载体来增强骨修复。在这项研究中,我们研究了基因在大鼠和人骨髓基质细胞中的转移,以评估自互补AAV载体(scAAV)系统的有效性,该系统比单链AAV载体(ssAAV)具有更高的效率,因为其独特的病毒基因组绕过了ssAAV所需的限制性转化步骤。方法:采用编码GFP和BMP-2的自互补yaav2 (scAAV2-GFP和scAAV2-BMP-2)体外转染人和大鼠骨髓基质细胞,在处理48h后检测GFP和BMP-2的表达水平。在平行实验中,采用腺病毒和慢病毒载体介导过表达GFP和BMP-2进行比较。结果:我们的研究结果表明,scAAV2在人和大鼠骨髓基质细胞中不能诱导显著的转基因表达,这可能与其独特的趋向性有关。结论:在开发离体基因治疗方案时,需要评估载体诱导适当水平的转基因表达的能力,以适应所使用的每种细胞类型和载体。
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