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Development and Applications of VSV Vectors Based on Cell Tropism

机译:基于细胞趋向性的VSV载体的开发与应用

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摘要

Viral vectors have been available in various fields such as medical and biological research or gene therapy applications. Targeting vectors pseudotyped with distinct viral envelope proteins that influence cell tropism and transfection efficiency are useful tools not only for examining entry mechanisms or cell tropisms but also for vaccine vector development. Vesicular stomatitis virus (VSV) is an excellent candidate for development as a pseudotype vector. A recombinant VSV lacking its own envelope (G) gene has been used to produce a pseudotype or recombinant VSV possessing the envelope proteins of heterologous viruses. These viruses possess a reporter gene instead of a VSV G gene in their genome, and therefore it is easy to evaluate their infectivity in the study of viral entry, including identification of viral receptors. Furthermore, advantage can be taken of a property of the pseudotype VSV, which is competence for single-round infection, in handling many different viruses that are either difficult to amplify in cultured cells or animals or that require specialized containment facilities. Here we describe procedures for producing pseudotype or recombinant VSVs and a few of the more prominent examples from envelope viruses, such as hepatitis C virus, Japanese encephalitis virus, baculovirus, and hemorrhagic fever viruses.
机译:病毒载体已在各个领域获得,例如医学和生物学研究或基因治疗应用。用影响细胞嗜性和转染效率的独特病毒包膜蛋白假型化的靶向载体不仅是检查进入机制或细胞嗜性的有用工具,而且还是疫苗载体开发的有用工具。水泡性口炎病毒(VSV)是作为假型载体发展的极佳候选者。缺乏自身包膜(G)基因的重组VSV已被用于产生具有异源病毒的包膜蛋白的假型或重组VSV。这些病毒在其基因组中具有报告基因而不是VSV G基因,因此在研究病毒进入研究(包括鉴定病毒受体)时很容易评估其感染性。此外,在处理许多不同的病毒时,可以利用伪型VSV的特性,该特性具有单轮感染的能力,这些病毒要么很难在培养的细胞或动物中扩增,要么需要专门的收容设施。在这里,我们描述了生产假型或重组VSV的程序,以及包膜病毒(例如丙型肝炎病毒,日本脑炎病毒,杆状病毒和出血热病毒)中一些更突出的例子。

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