Viral Replicon Systems and Their Biosafety Aspects.

IF 0.5 Q4 PUBLIC, ENVIRONMENTAL & OCCUPATIONAL HEALTH
Applied Biosafety Pub Date : 2023-06-01 Epub Date: 2023-06-05 DOI:10.1089/apb.2022.0037
Karen van der Meulen, Greet Smets, Patrick Rüdelsheim
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引用次数: 0

Abstract

Introduction: Viral RNA replicons are self-amplifying RNA molecules generated by deleting genetic information of one or multiple structural proteins of wild-type viruses. Remaining viral RNA is used as such (naked replicon) or packaged into a viral replicon particle (VRP), whereby missing genes or proteins are supplied via production cells. Since replicons mostly originate from pathogenic wild-type viruses, careful risk consideration is crucial.

Methods: A literature review was performed compiling information on potential biosafety risks of replicons originating from positive- and negative-sense single-stranded RNA viruses (except retroviruses).

Results: For naked replicons, risk considerations included genome integration, persistence in host cells, generation of virus-like vesicles, and off-target effects. For VRP, the main risk consideration was formation of primary replication competent virus (RCV) as a result of recombination or complementation. To limit the risks, mostly measures aiming at reducing the likelihood of RCV formation have been described. Also, modifying viral proteins in such a way that they do not exhibit hazardous characteristics in the unlikely event of RCV formation has been reported.

Discussion and conclusion: Despite multiple approaches developed to reduce the likelihood of RCV formation, scientific uncertainty remains on the actual contribution of the measures and on limitations to test their effectiveness. In contrast, even though effectiveness of each individual measure is unclear, using multiple measures on different aspects of the system may create a solid barrier. Risk considerations identified in the current study can also be used to support risk group assignment of replicon constructs based on a purely synthetic design.

病毒复制子系统及其生物安全问题。
引言病毒 RNA 复制子是通过删除野生型病毒的一种或多种结构蛋白的遗传信息而产生的自我扩增 RNA 分子。剩余的病毒 RNA 可作为复制子使用(裸体复制子),也可包装成病毒复制子颗粒(VRP),通过生产细胞提供缺失的基因或蛋白质。由于复制子大多来自致病性野生型病毒,因此仔细考虑风险至关重要:方法:对有关源自正义和负义单链 RNA 病毒(逆转录病毒除外)的复制子潜在生物安全风险的信息进行了文献综述:对于裸体复制子,风险考虑因素包括基因组整合、在宿主细胞中的持久性、病毒样囊泡的产生以及脱靶效应。对于 VRP,主要的风险考虑因素是重组或互补导致形成初级复制能力病毒(RCV)。为了限制风险,已经介绍了许多旨在降低 RCV 形成可能性的措施。此外,还有报告称,对病毒蛋白质进行改造,使其在万一形成 RCV 的情况下不会表现出危险特性:尽管已开发出多种方法来降低 RCV 形成的可能性,但这些措施的实际作用以及检验其有效性的局限性在科学上仍存在不确定性。相反,尽管每项措施的有效性尚不明确,但在系统的不同方面采用多种措施可能会形成一道坚实的屏障。当前研究中确定的风险考虑因素也可用于支持基于纯合成设计的复制子构建的风险组分配。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Applied Biosafety
Applied Biosafety Environmental Science-Management, Monitoring, Policy and Law
CiteScore
2.50
自引率
13.30%
发文量
27
期刊介绍: Applied Biosafety (APB), sponsored by ABSA International, is a peer-reviewed, scientific journal committed to promoting global biosafety awareness and best practices to prevent occupational exposures and adverse environmental impacts related to biohazardous releases. APB provides a forum for exchanging sound biosafety and biosecurity initiatives by publishing original articles, review articles, letters to the editors, commentaries, and brief reviews. APB informs scientists, safety professionals, policymakers, engineers, architects, and governmental organizations. The journal is committed to publishing on topics significant in well-resourced countries as well as information relevant to underserved regions, engaging and cultivating the development of biosafety professionals globally.
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