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Chimeric Measles Viruses with a Foreign Envelope

机译:带有异国信封的嵌合麻疹病毒

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摘要

Measles virus (MV) and vesicular stomatitis virus (VSV) are both members of the Mononegavirales but are only distantly related. We generated two genetically stable chimeric viruses. In MGV, the reading frames of the MV envelope glycoproteins H and F were substituted by a single reading frame encoding the VSV G glycoprotein; MG/FV is similar but encodes a G/F hybrid in which the VSV G cytoplasmic tail was replaced by that of MV F. In contrast to MG/FV, MGV virions do not contain the MV matrix (M) protein. This demonstrates that virus assembly is possible in the absence of M; conversely, the cytoplasmic domain of F allows incorporation of M and enhances assembly. The formation of chimeric viruses was substantially delayed and the titers obtained were reduced about 50-fold in comparison to standard MV. In the novel chimeras, transcription and replication are mediated by the MV ribonucleoproteins but the envelope glycoproteins dictate the host range. Mice immunized with the chimeric viruses were protected against lethal doses of wild-type VSV. These findings suggest that it is feasible to construct MV variants bearing a variety of different envelopes for use as vaccines or for gene therapeutic purposes.
机译:麻疹病毒(MV)和水疱性口炎病毒(VSV)都是Mononegavirales的成员,但只有很远的关联。我们产生了两种遗传稳定的嵌合病毒。在MGV中,MV包膜糖蛋白H和F的阅读框被编码VSV G糖蛋白的单个阅读框取代; MG / FV相似,但编码一个G / F杂种,其中VSV G的细胞质尾部被MV F替代。与MG / FV相比,MGV病毒体不含MV基质(M)蛋白。这表明在不存在M的情况下病毒组装是可能的。相反,F的胞质结构域允许M的掺入并增强装配。与标准MV相比,嵌合病毒的形成被大大延迟了,获得的效价降低了约50倍。在新型嵌合体中,转录和复制是由MV核糖核蛋白介导的,但包膜糖蛋白决定了宿主的范围。用嵌合病毒免疫的小鼠被保护免于致命剂量的野生型VSV。这些发现表明,构建带有多种不同包膜的MV变体作为疫苗或用于基因治疗目的是可行的。

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