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HIV-1基质蛋白在核衣壳区域的重新定位无法赋予病毒样颗粒组装能力。

HIV-1 matrix protein repositioning in nucleocapsid region fails to confer virus-like particle assembly.

作者信息

Chang Ching-Yuan, Chang Yu-Fen, Wang Shiu-Mei, Tseng Ying-Tzu, Huang Kuo-Jung, Wang Chin-Tien

机构信息

Department of Medical Research and Education, Taipei Veterans General Hospital, Institute of Clinical Medicine, National Yang-Ming University School of Medicine, Taipei, Taiwan.

出版信息

Virology. 2008 Aug 15;378(1):97-104. doi: 10.1016/j.virol.2008.05.010. Epub 2008 Jun 12.

Abstract

The HIV-1 matrix (MA) protein is similar to nucleocapsid (NC) proteins in its propensity for self-interaction and association with RNA. Here we report on our finding that replacing MA with NC results in the production of wild type (wt)-level RNA and virus-like particles (VLPs). In contrast, constructs containing MA as a substitute for NC are markedly defective in VLP production and form virions with lower densities than wt, even though their RNA content is over 50% that of wt level. We also noted that a DeltaMN mutant lacking both MA and NC produces a relatively higher amount of VLPs than those in which MA was substituted for NC. Although DeltaMN contains approximately 30% the RNA of wt, it still exhibits virion densities equal (or very similar) to those of wt. The data suggest that neither NC nor RNA are major virion density determinants. Furthermore, we noted that NC(ZIP)--a NC replacement with a leucine zipper dimerization motif--produces VLPs as efficiently as wt. However, the markedly reduced assembly efficiency of NC(ZIP) is associated with the formation of VLPs with densities slightly lower than those of wt following MA removal, suggesting that (a) MA is required to help the inserted leucine zipper motif perform efficient Gag multimerization, and (b) MA plays a role in the virus assembly process.

摘要

HIV-1基质(MA)蛋白在自我相互作用以及与RNA结合的倾向方面与核衣壳(NC)蛋白相似。在此我们报告我们的发现,即用NC替代MA会导致野生型(wt)水平的RNA和病毒样颗粒(VLP)产生。相比之下,含有MA替代NC的构建体在VLP产生方面存在明显缺陷,并且形成的病毒粒子密度低于wt,尽管其RNA含量超过wt水平的50%。我们还注意到,缺失MA和NC的DeltaMN突变体产生的VLP数量比用MA替代NC的构建体产生的VLP数量相对更多。尽管DeltaMN的RNA含量约为wt的30%,但其病毒粒子密度仍与wt相等(或非常相似)。这些数据表明,NC和RNA都不是主要的病毒粒子密度决定因素。此外,我们注意到,带有亮氨酸拉链二聚化基序的NC替代物NC(ZIP)产生VLP的效率与wt一样高。然而,NC(ZIP)显著降低的组装效率与去除MA后形成的密度略低于wt的VLP有关,这表明(a)MA是帮助插入的亮氨酸拉链基序进行有效的Gag多聚化所必需的,并且(b)MA在病毒组装过程中发挥作用。

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