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沙粒病毒减毒活疫苗研发的一般分子策略

General Molecular Strategy for Development of Arenavirus Live-Attenuated Vaccines.

作者信息

Iwasaki Masaharu, Ngo Nhi, Cubitt Beatrice, Teijaro John R, de la Torre Juan C

机构信息

Department of Immunology and Microbial Science, The Scripps Research Institute, La Jolla, California, USA.

Department of Immunology and Microbial Science, The Scripps Research Institute, La Jolla, California, USA

出版信息

J Virol. 2015 Dec;89(23):12166-77. doi: 10.1128/JVI.02075-15. Epub 2015 Sep 23.

Abstract

UNLABELLED

Hemorrhagic fever arenaviruses (HFA) pose important public health problems in regions where they are endemic. Thus, Lassa virus (LASV) infects several hundred thousand individuals yearly in West Africa, causing a large number of Lassa fever cases associated with high morbidity and mortality. Concerns about human-pathogenic arenaviruses are exacerbated because of the lack of FDA-licensed arenavirus vaccines and because current antiarenaviral therapy is limited to an off-label use of ribavirin that is only partially effective. The Mopeia virus (MOPV)/LASV reassortant (ML29) is a LASV candidate live-attenuated vaccine (LAV) that has shown promising results in animal models. Nevertheless, the mechanism of ML29 attenuation remains unknown, which raises concerns about the phenotypic stability of ML29 in response to additional mutations. Development of LAVs based on well-defined molecular mechanisms of attenuation will represent a major step in combatting HFA. We used the prototypic arenavirus lymphocytic choriomeningitis virus (LCMV) to develop a general molecular strategy for arenavirus attenuation. Our approach involved replacement of the noncoding intergenic region (IGR) of the L genome segment with the IGR of the S genome segment to generate a recombinant LCMV, rLCMV(IGR/S-S), that was highly attenuated in vivo but induced protection against a lethal challenge with wild-type LCMV. Attenuation of rLCMV(IGR/S-S) was associated with a stable reorganization of the control of viral gene expression. This strategy can facilitate the rapid development of LAVs with the antigenic composition of the parental HFA and a mechanism of attenuation that minimizes concerns about increased virulence that could be caused by genetic changes in the LAV.

IMPORTANCE

Hemorrhagic fever arenaviruses (HFA) cause high morbidity and mortality, and pose important public health problems in the regions where they are endemic. Implementation of live-attenuated vaccines (LAV) will represent a major step in combatting HFA. Here we have used the prototypic arenavirus LCMV to document a general molecular strategy for arenavirus attenuation that can facilitate the rapid development of safe and effective, as well as stable, LAV to combat HFA.

摘要

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出血热沙粒病毒(HFA)在其流行地区构成了重要的公共卫生问题。因此,拉沙病毒(LASV)每年在西非感染数十万个体,导致大量拉沙热病例,且发病率和死亡率很高。由于缺乏美国食品药品监督管理局(FDA)批准的沙粒病毒疫苗,以及目前的抗沙粒病毒疗法仅限于非标签使用的利巴韦林且效果有限,对人类致病的沙粒病毒的担忧加剧。莫佩亚病毒(MOPV)/拉沙病毒重组体(ML29)是一种拉沙病毒减毒活疫苗(LAV)候选疫苗,已在动物模型中显示出有前景的结果。然而,ML29减毒的机制仍然未知,这引发了对ML29在应对额外突变时表型稳定性的担忧。基于明确的减毒分子机制开发减毒活疫苗将是对抗HFA的重要一步。我们使用原型沙粒病毒淋巴细胞性脉络丛脑膜炎病毒(LCMV)来制定沙粒病毒减毒的通用分子策略。我们的方法包括用S基因组片段的基因间隔区(IGR)替换L基因组片段的非编码基因间隔区,以产生重组LCMV,即rLCMV(IGR/S-S),其在体内高度减毒,但能诱导对野生型LCMV致死性攻击的保护作用。rLCMV(IGR/S-S)的减毒与病毒基因表达控制的稳定重组有关。该策略可促进具有亲本HFA抗原组成且减毒机制能将对减毒活疫苗基因变化可能导致毒力增加的担忧降至最低的减毒活疫苗的快速开发。

重要性

出血热沙粒病毒(HFA)导致高发病率和死亡率,在其流行地区构成重要的公共卫生问题。实施减毒活疫苗(LAV)将是对抗HFA的重要一步。在此,我们使用原型沙粒病毒LCMV记录了一种沙粒病毒减毒的通用分子策略,该策略可促进快速开发安全、有效且稳定的减毒活疫苗以对抗HFA。

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