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猴泡沫病毒Gag前体中的独立装配和运输结构域。

Separate assembly and transport domains within the Gag precursor of Mason-Pfizer monkey virus.

作者信息

Sakalian M, Hunter E

机构信息

Department of Microbiology, The University of Alabama at Birmingham, Birmingham, Alabama 35294, USA.

出版信息

J Virol. 1999 Oct;73(10):8073-82. doi: 10.1128/JVI.73.10.8073-8082.1999.

Abstract

Mason-Pfizer monkey virus (M-PMV), the prototypical type D retrovirus, assembles immature capsids within the cytoplasm of the cell prior to plasma membrane interaction. Several mutants of M-PMV Gag have been described which display altered transport, assembly, or both. In this report, we describe the use of an in vitro synthesis and assembly system to distinguish between defects in intracellular transport and the process of assembly itself for two previously described gag gene mutants. Matrix domain mutant R55W converts the type D morphogenesis of M-PMV particles into type C and has been hypothesized to alter the transport of Gag, redirecting it to the plasma membrane where assembly subsequently occurs. We show here that R55W can assemble in both the in vitro translation-assembly system and within inclusion bodies in bacteria and thus has retained the capacity to assemble in the cytoplasm. This supports the concept that R55 is located within a domain responsible for the transport of Gag to an intracellular site for assembly. In contrast, deletions within the p12 domain of M-PMV Gag had previously been shown to affect the efficiency of particle formation such that under low-level expression conditions, Gag would fail to assemble. We demonstrate here that the efficiency of assembly in the in vitro system mirrors that seen in cells under expression conditions similar to that of an infection. These results argue that the p12 domain of this D-type retrovirus plays a critical role in the membrane-independent assembly of immature capsids.

摘要

梅森- Pfizer猴病毒(M-PMV)是典型的D型逆转录病毒,在与质膜相互作用之前在细胞胞质内组装未成熟衣壳。已经描述了几种M-PMV Gag突变体,它们表现出运输、组装或两者的改变。在本报告中,我们描述了使用体外合成和组装系统来区分两种先前描述的gag基因突变体在细胞内运输和组装过程本身的缺陷。基质结构域突变体R55W将M-PMV颗粒的D型形态发生转变为C型,并且据推测会改变Gag的运输,将其重新导向随后发生组装的质膜。我们在此表明,R55W可以在体外翻译-组装系统以及细菌的包涵体内组装,因此保留了在细胞质中组装的能力。这支持了R55位于负责将Gag运输到细胞内组装位点的结构域内的概念。相比之下,先前已表明M-PMV Gag的p12结构域内的缺失会影响颗粒形成的效率,使得在低水平表达条件下,Gag无法组装。我们在此证明,体外系统中的组装效率反映了在类似于感染的表达条件下细胞中的情况。这些结果表明,这种D型逆转录病毒的p12结构域在未成熟衣壳的非膜依赖性组装中起关键作用。

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