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Replication-deficient human adenovirus type 35 vectors for gene transfer and vaccination: efficient human cell infection and bypass of preexisting adenovirus immunity

机译:用于基因转移和疫苗接种的复制缺陷型人类35型腺病毒载体:有效的人类细胞感染和绕过预先存在的腺病毒免疫

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摘要

Replication-deficient human adenovirus type 5 (Ad5) can be produced to high titers in complementing cell lines, such as PER.C6, and is widely used as a vaccine and gene therapy vector. However, preexisting immunity against Ad5 hampers consistency of gene transfer, immunological responses, and vector-mediated toxicities. We report the identification of human Ad35 as a virus with low global prevalence and the generation of an Ad35 vector plasmid system for easy insertion of heterologous genes. In addition, we have identified the minimal sequence of the Ad35-E1B region (molecular weight, 55,000 [55K]), pivotal for complementation of fully E1-lacking Ad35 vector on PER.C6 cells. After stable insertion of the 55K sequence into PER.C6 cells a cell line was obtained (PER.C6/55K) that efficiently transcomplements both Ad5 and Ad35 vectors. We further demonstrate that transduction with Ad35 is not hampered by preexisting Ad5 immunity and that Ad35 efficiently infects dendritic cells, smooth muscle cells, and synoviocytes, in contrast to Ad5
机译:复制缺陷型5型人类腺病毒(Ad5)可以在互补细胞系(如PER.C6)中产生高滴度,并广泛用作疫苗和基因治疗载体。但是,先前针对Ad5的免疫会影响基因转移,免疫应答和载体介导的毒性的一致性。我们报告了人类Ad35作为低全球患病率的病毒的鉴定和易于插入异源基因的Ad35矢量质粒系统的生成。此外,我们已经确定了Ad35-E1B区的最小序列(分子量,55,000 [55K]),对于PER.C6细胞上完全缺少E1的Ad35载体的互补至关重要。将55K序列稳定插入PER.C6细胞后,获得了一个细胞系(PER.C6 / 55K),可以有效地对Ad5和Ad35载体进行互补。我们进一步证明,与Ad5相比,Ad35的转导不会受到预先存在的Ad5免疫的阻碍,并且Ad35有效感染树突状细胞,平滑肌细胞和滑膜细胞

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