腺病毒HI环的噬菌体展示,用于“上下文特异性”配体选择

D. Ghosh, M. Barry
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引用次数: 0

摘要

腺病毒被用作基因治疗的传递载体,主要是因为它们能够有效地感染分裂细胞和非分裂细胞。然而,由于其对非靶向细胞类型的倾向,它们的成功受到阻碍。腺病毒可以通过添加配体来获得特异性。噬菌体呈递随机肽库已被用于选择潜在的配体。这种方法不需要细胞生物学的知识。然而,选定的肽工程进入腺病毒可以降低病毒衣壳功能,并且腺病毒可以削弱选定肽的靶向能力。我们的研究重点是开发用于配体选择的“上下文特定”随机文库。通过引入病毒背景,我们希望选择一种可以引入病毒而不影响功能的肽。在本文中,我们报道了腺病毒HI环内生物素受体肽的噬菌体展示(标记为HI- bap)。HI-BAP在丝状噬菌体的pIII次要外壳蛋白上表达并酶促生物素化。这种方法可以提高病毒载体的靶向性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Phage display of adenoviral HI loop for "context-specific" ligand selection
Adenoviruses are used as delivery vectors in gene therapy mainly due to their ability to efficiently infect dividing and non-dividing cells. However, their success is hindered due to its tropism for non-targeted cell types. Adenoviruses can be genetically retargeted by ligand addition to confer specificity. Phage-presenting random peptide libraries have been used to select potential ligands. This approach does not require knowledge of the cell biology. However, selected peptides engineered into the adenovirus can reduce viral capsid function, and the adenovirus can impair targeting ability of the selected peptide. Our research focuses on the development of "context-specific" random libraries for ligand selection. By introducing a viral context, we hope to select a peptide that can be introduced into the virus without affecting function. In this paper, we report the phage display of biotin acceptor peptide within the adenoviral HI loop (denoted HI-BAP). HI-BAP is expressed and enzymatically biotinylated on the pIII minor coat protein of filamentous phage. This approach can improve targeting of viral vectors.
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