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Adenovirus Serotype 5 Vectors with Tat-PTD Modified Hexon and Serotype 35 Fiber Show Greatly Enhanced Transduction Capacity of Primary Cell Cultures

机译:具有Tat-PTD修饰的六邻体和35型纤维的腺病毒5型血清载体显示出大大增强的原代细胞培养物转导能力

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摘要

Recombinant adenovirus serotype 5 (Ad5) vectors represent one of the most efficient gene delivery vectors in life sciences. However, Ad5 is dependent on expression of the coxsackievirus-adenovirus- receptor (CAR) on the surface of target cell for efficient transduction, which limits it's utility for certain cell types. Herein we present a new vector, Ad5PTDf35, which is an Ad5 vector having serotype 35 fiber-specificity and Tat-PTD hexon-modification. This vector shows dramatically increased transduction capacity of primary human cell cultures including T cells, monocytes, macrophages, dendritic cells, pancreatic islets and exocrine cells, mesenchymal stem cells and tumor initiating cells. Biodistribution in mice following systemic administration (tail-vein injection) show significantly reduced uptake in the liver and spleen of Ad5PTDf35 compared to unmodified Ad5. Therefore, replication-competent viruses with these modifications may be further developed as oncolytic agents for cancer therapy. User-friendly backbone plasmids containing these modifications were developed for compatibility to the AdEasy-system to facilitate the development of surface-modified adenoviruses for gene delivery to difficult-to-transduce cells in basic, pre-clinical and clinical research.
机译:重组腺病毒血清型5(Ad5)载体代表了生命科学中最有效的基因传递载体之一。但是,Ad5依赖于柯萨奇病毒-腺病毒-受体(CAR)在靶细胞表面的表达来进行有效的转导,这限制了它在某些细胞类型中的用途。在此,我们提出了一种新的载体Ad5PTDf35,它是具有血清型35纤维特异性和Tat-PTD六邻体修饰的Ad5载体。该载体显示了包括T细胞,单核细胞,巨噬细胞,树突细胞,胰岛和外分泌细胞,间充质干细胞和肿瘤起始细胞在内的人类原代细胞培养物的转导能力显着提高。与未经修饰的Ad5相比,全身给药(尾静脉注射)后小鼠体内的生物分布显示Ad5PTDf35在肝脏和脾脏中的摄取显着降低。因此,具有这些修饰的具有复制能力的病毒可以进一步开发为用于癌症治疗的溶瘤剂。已开发出包含这些修饰的用户友好型骨架质粒,以与AdEasy系统兼容,从而在基础,临床前和临床研究中促进表面修饰的腺病毒的开发,以便将基因传递至难以转导的细胞。

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