Alphavirus vectors and vaccination

α病毒 复制子 生物 亚基因组mRNA 病毒学 核糖核酸 异源的 基因 辛德比斯病毒 塞姆利基森林病毒 病毒 遗传学 质粒
作者
Jonathan O. Rayner,Sergey A. Dryga,Kurt I. Kamrud
出处
期刊:Reviews in Medical Virology [Wiley]
卷期号:12 (5): 279-296 被引量:178
标识
DOI:10.1002/rmv.360
摘要

Abstract Alphaviruses are positive‐stranded RNA viruses that have a broad host range and therefore are capable of replicating in many vertebrate and invertebrate cells. The single‐stranded alphavirus genome is divided into two ORFs. The first ORF encodes the nonstructural proteins that are translated upon entry of the virus into the cytoplasm and are responsible for transcription and replication of viral RNA. The second ORF is under the control of a subgenomic promoter and normally encodes the structural proteins, which are responsible for encapsidation of viral RNA and final assembly into enveloped particles. Expression vectors have been engineered from at least three alphaviruses in which the structural protein gene region has been replaced by heterologous genes and have been shown to express high levels of the heterologous protein in cultured cells. These RNA vectors, known as replicons, are capable of replicating on their own but are not packaged into virus‐like particles unless the structural proteins are provided in trans . Thus, replicons are single cycle vectors incapable of spreading from infected to noninfected cells. Because of these features, alphavirus replicon vectors are being developed as a platform vaccine technology for numerous viral, bacterial, protozoan and tumour antigens where they have been shown to be efficient inducers of both humoral and T cell responses. In addition, as the alphavirus structural proteins are not expressed in vaccine recipients, antivector immune responses are generally minimal, allowing for multiple effective immunisations of the same individual. Copyright © 2002 John Wiley & Sons, Ltd.
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