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痘病毒/逆转录病毒嵌合载体可在细胞质中产生具有转导能力的缺陷型逆转录病毒颗粒。

Poxviral/retroviral chimeric vectors allow cytoplasmic production of transducing defective retroviral particles.

作者信息

Holzer G W, Mayrhofer J A, Gritschenberger W, Dorner F, Falkner F G

机构信息

Biomedical Research Center, Baxter/Hyland Immuno Division, Uferstrasse 15, Orth/Donau, A-2304, Austria.

出版信息

Virology. 1999 Jan 5;253(1):107-14. doi: 10.1006/viro.1998.9496.

Abstract

Defective vaccinia viruses were constructed that express functional Moloney murine leukemia virus-based vector genomes, giving rise to substantial titers of transduction-competent retrovirus particles after infection of a retroviral packaging cell line. For this purpose, the proviral retrovirus genome, engineered into the vaccinia virus mutant, was subjected to several modifications, including the replacement of retroviral promoter sequences by vaccinia virus sequences and the precise fusion of the transcription stop signal downstream of and the removal of such signals within the transcription unit, allowing cytoplasmic transcription of distinct full-length retroviral transcripts. Vaccinia-mediated expression of retroviral vector particles could be observed as early as 3 h postinfection and resulted in stable transduction of NIH/3T3 target cells at higher titers than the control performed by conventional plasmid transfections. Thus at least part of the vaccinia life cycle and retroviral assembly can occur concomitantly. Due to the favorable properties of vaccinia vectors, including high coding capacity, stability, and wide host range, defective vaccinia viral/retroviral chimeric vectors are promising tools for gene therapy applications.

摘要

构建了缺陷型痘苗病毒,其表达基于莫洛尼鼠白血病病毒的功能性载体基因组,在感染逆转录病毒包装细胞系后产生大量具有转导能力的逆转录病毒颗粒。为此,将工程化到痘苗病毒突变体中的前病毒逆转录病毒基因组进行了多项修饰,包括用痘苗病毒序列替换逆转录病毒启动子序列,以及精确融合转录单位下游的转录终止信号并去除转录单位内的此类信号,从而允许不同全长逆转录病毒转录本在细胞质中进行转录。痘苗介导的逆转录病毒载体颗粒的表达最早可在感染后3小时观察到,并导致NIH/3T3靶细胞以比传统质粒转染更高的滴度进行稳定转导。因此,痘苗生命周期和逆转录病毒组装的至少一部分可以同时发生。由于痘苗载体具有诸如高编码能力、稳定性和广泛宿主范围等有利特性,缺陷型痘苗病毒/逆转录病毒嵌合载体是基因治疗应用中有前景的工具。

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