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通过将单链或单域抗体与衣壳蛋白 IX 进行基因融合来重新定向腺病毒载体。

Retargeting of adenovirus vectors through genetic fusion of a single-chain or single-domain antibody to capsid protein IX.

机构信息

Regenerative Medicine Program, Ottawa Hospital Research Institute, Ottawa, Ontario, Canada.

出版信息

J Virol. 2010 Oct;84(19):10074-86. doi: 10.1128/JVI.02665-09. Epub 2010 Jul 14.

Abstract

Adenovirus (Ad) vectors are the most commonly used system for gene therapy applications, due in part to their ability to infect a wide array of cell types and tissues. However, many therapies would benefit from the ability to target the Ad vector only to specific cells, such as tumor cells for cancer gene therapy. In this study, we investigated the utility of capsid protein IX (pIX) as a platform for the presentation of single-chain variable-fragment antibodies (scFv) and single-domain antibodies (sdAb) for virus retargeting. We show that scFv can be displayed on the capsid through genetic fusion to native pIX but that these molecules fail to retarget the virus, due to improper folding of the scFv. Redirecting expression of the fusion protein to the endoplasmic reticulum (ER) results in correct folding of the scFv and allows it to recognize its epitope; however, ER-targeted pIX-scFv was incorporated into the Ad capsid at a very low level which was not sufficient to retarget virus infection. In contrast, a pIX-sdAb construct was efficiently incorporated into the Ad capsid and enhanced virus infection of cells expressing the targeted receptor. Taken together, our data indicate that pIX is an effective platform for presentation of large targeting polypeptides on the surface of the virus capsid, but the nature of the ligand can significantly affect its association with virions.

摘要

腺病毒 (Ad) 载体是基因治疗应用中最常用的系统,部分原因是它们能够感染广泛的细胞类型和组织。然而,许多治疗方法将受益于仅将 Ad 载体靶向特定细胞的能力,例如癌症基因治疗中的肿瘤细胞。在这项研究中,我们研究了衣壳蛋白 IX (pIX) 作为展示单链可变片段抗体 (scFv) 和单域抗体 (sdAb) 用于病毒重定向的平台的实用性。我们表明,scFv 可以通过与天然 pIX 的基因融合展示在衣壳上,但由于 scFv 的不正确折叠,这些分子未能重新靶向病毒。将融合蛋白的表达重定向到内质网 (ER) 会导致 scFv 的正确折叠,并使其能够识别其表位;然而,靶向 ER 的 pIX-scFv 以非常低的水平掺入 Ad 衣壳,不足以重新靶向病毒感染。相比之下,pIX-sdAb 构建体有效地掺入 Ad 衣壳并增强了表达靶向受体的细胞的病毒感染。总之,我们的数据表明 pIX 是在病毒衣壳表面展示大型靶向多肽的有效平台,但配体的性质会显著影响其与病毒粒子的结合。

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