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High-Density Recombinant Adeno-Associated Viral Particles are Competent Vectors for In Vivo Transduction

机译:高密度重组腺相关病毒颗粒是体内转导的感受态载体

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摘要

Recombinant adeno-associated viral (rAAV) vectors have recently achieved clinical successes in human gene therapy. However, the commonly observed, heavier particles found in rAAV preparations have traditionally been ignored due to their reported low in vitro transduction efficiency. In this study, the biological properties of regular and high-density rAAV serotype 8 vectors, rAAV(RD) and rAAV(HD), were systemically compared. Results demonstrated that both rAAV(RD) and rAAV(HD) exhibited similar DNA packaging profiles, while rAAV(HD) capsids contained fewer VP1 and VP2 proteins, indicating that the rAAV(HD) particles contained a higher DNA/protein ratio than that of rAAV(RD) particles. Dynamic light scattering and transmission electron microscopy data revealed that the diameter of rAAV(HD) was smaller than that of rAAV(RD). In vitro, rAAV(HD) was two-to fourfold less efficient in transduction compared with rAAV(RD). However, the transduction performance of rAAV(HD) and rAAV(RD) was similar in vivo. No significant difference in neutralizing antibody formation against rAAV(RD) and rAAV(HD) was observed, suggesting that the surface epitopes of rAAV(RD) and rAAV(HD) are congruent. In summary, the results of this study demonstrate that rAAV(RD) and rAAV(HD) are equally competent for in vivo transduction, despite their difference in vitro. Therefore, the use of rAAV(HD) vectors in human gene therapy should be further evaluated.
机译:重组腺相关病毒(rAAV)载体最近在人类基因治疗中取得了临床成功。然而,在rAAV制剂中发现的常见较重颗粒传统上被忽略,因为它们的体外转导效率较低。本研究对常规和高密度rAAV血清型8载体rAAV(RD)和rAAV(HD)的生物学特性进行了系统比较。结果表明,rAAV(RD)和rAAV(HD)的DNA包装特征相似,而rAAV(HD)衣壳中VP1和VP2蛋白含量较低,表明rAAV(HD)颗粒的DNA/蛋白质比值高于rAAV(RD)颗粒。动态光散射和透射电子显微镜数据显示,rAAV(HD)的直径小于rAAV(RD)。在体外,rAAV(HD)的转导效率比rAAV(RD)低2至4倍。然而,rAAV(HD)和rAAV(RD)在体内的转导性能相似。在针对rAAV(RD)和rAAV(HD)的中和抗体形成方面没有显著差异,表明rAAV(RD)和rAAV(HD)的表面表位是一致的。总之,本研究的结果表明,尽管 rAAV(RD) 和 rAAV(HD) 在体外存在差异,但它们对体内转导具有同等能力。因此,应进一步评估rAAV(HD)载体在人类基因治疗中的应用。

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