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一种利用T7 RNA聚合酶的甲型流感病毒反向遗传学系统。

A reverse-genetics system for Influenza A virus using T7 RNA polymerase.

作者信息

de Wit Emmie, Spronken Monique I J, Vervaet Gaby, Rimmelzwaan Guus F, Osterhaus Albert D M E, Fouchier Ron A M

机构信息

Solvay Pharmaceuticals BV, Weesp, The Netherlands.

National Influenza Center, Department of Virology and Postgraduate School of Molecular Medicine, Erasmus MC, PO Box 1738, 3000 DR Rotterdam, The Netherlands.

出版信息

J Gen Virol. 2007 Apr;88(Pt 4):1281-1287. doi: 10.1099/vir.0.82452-0.

Abstract

The currently available reverse-genetics systems for Influenza A virus are all based on transcription of genomic RNA by RNA polymerase I, but the species specificity of this polymerase is a disadvantage. A reverse-genetics vector containing a T7 RNA polymerase promoter, hepatitis delta virus ribozyme sequence and T7 RNA polymerase terminator sequence has been developed. To achieve optimal expression in minigenome assays, it was determined that viral RNA should be inserted in this vector in the negative-sense orientation with two additional G residues downstream of the T7 RNA polymerase promoter. It was also shown that expression of the minigenome was more efficient when a T7 RNA polymerase with a nuclear-localization signal was used. By using this reverse-genetics system, recombinant influenza virus A/PR/8/34 was produced more efficiently than by using a similar polymerase I-based reverse-genetics system. Furthermore, influenza virus A/NL/219/03 could be rescued from 293T, MDCK and QT6 cells. Thus, a reverse-genetics system for the rescue of Influenza A virus has been developed, which will be useful for fundamental research and vaccine seed strain production in a variety of cell lines.

摘要

目前可用的甲型流感病毒反向遗传学系统均基于RNA聚合酶I对基因组RNA的转录,但该聚合酶的物种特异性是一个缺点。已开发出一种包含T7 RNA聚合酶启动子、丁型肝炎病毒核酶序列和T7 RNA聚合酶终止子序列的反向遗传载体。为了在微型基因组检测中实现最佳表达,确定应将病毒RNA以负义方向插入该载体,并在T7 RNA聚合酶启动子下游添加两个额外的G残基。还表明,使用带有核定位信号的T7 RNA聚合酶时,微型基因组的表达效率更高。通过使用这种反向遗传学系统,重组甲型流感病毒A/PR/8/34的产生效率比使用类似的基于聚合酶I的反向遗传学系统更高。此外,甲型流感病毒A/NL/219/03可从293T、MDCK和QT6细胞中拯救出来。因此,已开发出一种用于拯救甲型流感病毒的反向遗传学系统,这将有助于在多种细胞系中进行基础研究和疫苗种子株的生产。

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