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携带优化的双顺反子NA片段及延长的天然5'末端序列的重组甲型流感病毒:在小鼠中诱导异源特异性B细胞和T细胞反应

Recombinant influenza A viruses harboring optimized dicistronic NA segment with an extended native 5' terminal sequence: induction of heterospecific B and T cell responses in mice.

作者信息

Vieira Machado Alexandre, Naffakh Nadia, Gerbaud Sylvie, van der Werf Sylvie, Escriou Nicolas

机构信息

Unité de Génétique Moléculaire des Virus Respiratoires, URA 1966 CNRS, Institut Pasteur, 25 rue du Dr. Roux, 75724 Paris Cedex 15, France.

出版信息

Virology. 2006 Feb 5;345(1):73-87. doi: 10.1016/j.virol.2005.09.050. Epub 2005 Nov 3.

Abstract

We generated novel recombinant influenza A viruses (vNA38) harboring dicistronic NA segments with an extended native 5' terminal sequence of 70 nucleotides comprised of the last 42 nucleotides of the NA ORF and the 5' noncoding region (5' NCR). vNA38 viruses replicated stably and more efficiently than vNA35 viruses with a dicistronic NA segment comprised of the native 5' NCR only, that we described previously (Vieira Machado, A., Naffakh, N., van der Werf, S., Escriou, N., 2003. Expression of a foreign gene by stable recombinant influenza viruses harboring a dicistronic genomic segment with an internal promoter. Virology 313, 235-249). In addition, vNA38 viruses drove the expression of higher levels of encoded heterologous proteins than corresponding vNA35 viruses, both in cell culture and in the pulmonary tissue of infected mice. These data demonstrate that a sequence overlapping 5' coding and noncoding regions of the NA segment determines efficient replication and/or propagation of the vRNA. Intranasal immunization of mice with live vNA38 viruses induced B and T cell responses specific for the heterologous protein expressed, establishing the usefulness of such recombinant influenza viruses with a dicistronic segment for the development of live bivalent vaccines.

摘要

我们构建了新型重组甲型流感病毒(vNA38),其携带双顺反子NA片段,该片段具有由NA开放阅读框(ORF)的最后42个核苷酸和5'非编码区(5' NCR)组成的70个核苷酸的延长天然5'末端序列。vNA38病毒比仅具有由天然5' NCR组成的双顺反子NA片段的vNA35病毒更稳定且更高效地复制,vNA35病毒是我们之前描述过的(Vieira Machado, A., Naffakh, N., van der Werf, S., Escriou, N., 2003. Expression of a foreign gene by stable recombinant influenza viruses harboring a dicistronic genomic segment with an internal promoter. Virology 313, 235 - 249)。此外,在细胞培养和感染小鼠的肺组织中,vNA38病毒驱动表达的编码异源蛋白水平高于相应的vNA35病毒。这些数据表明,与NA片段的5'编码区和非编码区重叠的序列决定了vRNA的有效复制和/或传播。用活的vNA38病毒对小鼠进行鼻内免疫可诱导针对所表达异源蛋白的B细胞和T细胞反应,证实了这种具有双顺反子片段的重组流感病毒在开发活二价疫苗方面的实用性。

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