首页> 外文期刊>Journal of orthopaedic research >Effect of transfection strategy on growth factor overexpression by articular chondrocytes.
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Effect of transfection strategy on growth factor overexpression by articular chondrocytes.

机译:转染策略对关节软骨细胞生长因子过度表达的影响。

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Articular cartilage damage remains an unsolved problem in orthopaedics. Insulin-like growth factor I (IGF-I) and fibroblast growth factor-2 (FGF-2) are anabolic and mitogenic for articular chondrocytes, and are candidates for the application of gene therapy to articular cartilage repair. We tested the hypothesis that the production of IGF-I and FGF-2 can be augmented by modulating vector designs and delivery methods used for gene transfer to articular chondrocytes. We developed a novel adeno-associated virus (AAV)-based plasmid (pAAV) to overexpress IGF-I and FGF-2 cDNAs in adult bovine articular chondrocytes. We found that the pAAV-based vectors generated significantly more growth factor than pcDNA vectors carrying the same cDNAs. Chondrocytes cotransfected with both IGF-I and FGF-2 cDNAs in two separate pAAV plasmids produced significantly more IGF-I and FGF-2 than cells transfected by a single pAAV plasmid carrying both cDNAs in a dicistronic cassette. These data indicate that pAAV vectors are more effective than pcDNA vectors for transfer of IGF-I and FGF-2 genes to articular chondrocytes. They further suggest that cotransfection may be an effective strategy for multiple gene transfer to these cells. These findings may be important in applying growth factor gene transfer to cell-based articular cartilage gene therapy.
机译:关节软骨损伤仍然是骨科中尚未解决的问题。胰岛素样生长因子I(IGF-1)和成纤维细胞生长因子2(FGF-2)对关节软骨细胞具有合成代谢和促有丝分裂作用,是将基因疗法应用于关节软骨修复的候选药物。我们测试了这样的假设,即通过调节用于基因转移至关节软骨细胞的载体设计和递送方法,可以增加IGF-1和FGF-2的产量。我们开发了一种新型的腺相关病毒(AAV)为基础的质粒(pAAV)在成年牛关节软骨细胞中过表达IGF-I和FGF-2 cDNA。我们发现基于pAAV的载体比带有相同cDNA的pcDNA载体产生的生长因子明显更多。在两个单独的pAAV质粒中与IGF-1和FGF-2 cDNA共转染的软骨细胞比在双顺反子盒中被单个带有两个cDNA的pAAV质粒转染的细胞产生的IGF-1和FGF-2明显多。这些数据表明,pAAV载体比pcDNA载体更有效地将IGF-1和FGF-2基因转移至关节软骨细胞。他们进一步表明,共转染可能是将多个基因转移至这些细胞的有效策略。这些发现对于将生长因子基因转移应用于基于细胞的关节软骨基因治疗可能是重要的。

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