Muriaux Delphine, Costes Sylvain, Nagashima Kunio, Mirro Jane, Cho Ed, Lockett Stephen, Rein Alan
HIV Drug Resistance Program, National Cancer Institute-Frederick, P.O. Box B, Frederick, MD 21702-1201, USA.
J Virol. 2004 Nov;78(22):12378-85. doi: 10.1128/JVI.78.22.12378-12385.2004.
The retroviral nucleocapsid protein (NC) originates by cleavage of the Gag polyprotein. It is highly basic and contains one or two zinc fingers. Mutations in either the basic residues or the zinc fingers can affect several events of the virus life cycle. They frequently prevent the specific packaging of the viral RNA, affect reverse transcription, and impair virion assembly. In this work, we explore the role of NC in murine leukemia virus (MLV) particle assembly and release. A panel of NC mutants, including mutants of the zinc finger and of a basic region, as well as truncations of the NC domain of Gag, were studied. Several of these mutations dramatically reduce the release of virus particles. A mutant completely lacking the NC domain is apparently incapable of assembling into particles, although its Gag protein is still targeted to the plasma membrane. By electron microscopy on thin sections of virus-producing cells, we observed that some NC mutants exhibit various stages of budding defects at the plasma membrane and have aberrant particle morphology; electron micrographs of cells expressing some of these mutants are strikingly similar to those of cells expressing "late-domain" mutants. However, the defects of NC mutants with respect to virus release and infectivity could be complemented by an MLV lacking the p12 domain. Therefore, the functions of NC in virus budding and infectivity are completely distinct from viral late-domain function.
逆转录病毒核衣壳蛋白(NC)由Gag多蛋白裂解产生。它具有高度碱性,包含一个或两个锌指结构。碱性残基或锌指结构中的突变会影响病毒生命周期的多个事件。这些突变常常会阻止病毒RNA的特异性包装,影响逆转录,并损害病毒粒子的组装。在这项研究中,我们探讨了NC在小鼠白血病病毒(MLV)粒子组装和释放中的作用。我们研究了一组NC突变体,包括锌指结构和一个碱性区域的突变体,以及Gag的NC结构域的截短突变体。其中一些突变显著降低了病毒粒子的释放。一个完全缺失NC结构域的突变体显然无法组装成粒子,尽管其Gag蛋白仍靶向质膜。通过对产生病毒的细胞超薄切片进行电子显微镜观察,我们发现一些NC突变体在质膜处表现出不同阶段的出芽缺陷,并且具有异常的粒子形态;表达其中一些突变体的细胞的电子显微镜照片与表达“晚期结构域”突变体的细胞的照片惊人地相似。然而,缺乏p12结构域的MLV可以弥补NC突变体在病毒释放和感染性方面的缺陷。因此,NC在病毒出芽和感染性方面的功能与病毒晚期结构域的功能完全不同。