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Transduction Efficiencies of Novel AAV Vectors in Mouse Airway Epithelium In Vivo and Human Ciliated Airway Epithelium In Vitro

机译:新型AAV载体在小鼠气管上皮和人纤毛气管上皮中的转导效率

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摘要

We have characterized the ability of adeno-associated virus (AAV) serotypes 1–9 in addition to nineteen novel vectors isolated from various tissues, to transduce mouse and human ciliated airway epithelium (HAE). Vectors expressing α-1-antitrypsin (AAT) and β-galactosidase were co-instilled into the mouse lung. Of all the vectors tested rh.64R1, AAV5 and AAV6 were the most efficient. The high transduction observed in mouse was reproduced in HAE cell cultures for both rh.64R1 and AAV6 but not for AAV5. Since AAV6 was the most efficient vector in mouse and HAE we also tested the transduction efficiencies of the AAV6 singleton vectors (i.e., AAV6 variants with targeted mutations) in these models. Of these, AAV6.2 transduced mouse airway epithelium and HAE with greater efficiency than all other AAV vectors tested. We demonstrated that AAV6.2 exhibits improved transduction efficiency compared to previously reported AAVs in mouse airways and in culture models of human airway epithelium and that this vector requires further development for preclinical and clinical testing.
机译:除了从各种组织中分离出的十九种新型载体外,我们还表征了1-9型腺伴随病毒(AAV)的能力,以转导小鼠和人纤毛气管上皮(HAE)。将表达α-1-抗胰蛋白酶(AAT)和β-半乳糖苷酶的载体共滴入小鼠肺。在所有经测试的载体中,rh.64R1,AAV5和AAV6效率最高。在鼠中观察到的高转导在rhE64R1和AAV6的HAE细胞培养物中均得到了复制,但对于AAV5却没有。由于AAV6是小鼠和HAE中最有效的载体,因此我们还在这些模型中测试了AAV6单例载体(即具有目标突变的AAV6变体)的转导效率。其中,AAV6.2转导的小鼠气道上皮和HAE比所有其他测试的AAV载体效率更高。我们证明,与以前报道的AAVs在小鼠气道和人气道上皮细胞培养模型中相比,AAV6.2表现出更高的转导效率,并且该载体需要进一步开发以用于临床前和临床测试。

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