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猫免疫缺陷病毒和猿猴免疫缺陷病毒基质蛋白之间的功能关系。

Functional relationship between the matrix proteins of feline and simian immunodeficiency viruses.

作者信息

Manrique Mariana L, González Silvia A, Affranchino José L

机构信息

Centro de Virología Animal (CEVAN-CONICET), C1414DEM Buenos Aires, Argentina.

出版信息

Virology. 2004 Nov 10;329(1):157-67. doi: 10.1016/j.virol.2004.07.029.

Abstract

To investigate the functional relationship between the matrix (MA) proteins of feline and simian immunodeficiency viruses (FIV and SIV, respectively), we generated chimeric proviruses in which the MA-coding region of an SIV infectious molecular clone was partially or fully replaced by its FIV counterpart. Chimeric SIV proviruses containing the amino-terminal 36 residues or the central and carboxy-terminal regions of the FIV MA assembled into virions as efficiently as wild-type SIV. However, the resulting virions were noninfectious in single-cycle infectivity assays. Furthermore, a chimeric SIV provirus containing the entire FIV MA was found to be severely impaired in virion production due to inefficient membrane binding of the chimeric Gag polyprotein. Interestingly, the assembly defective phenotype of this chimeric Gag precursor could be reversed either by introducing the G31K/G33K double amino acid substitution in the FIV-derived MA domain or by coexpression with wild-type SIV Gag. Of note, a chimeric FIV provirus expressing the SIV MA not only assembled into particles as efficiently as wild-type FIV, but also replicated in feline T cells with wild-type kinetics. Our results thus provide novel information about the functional homology between the MA proteins of distantly related lentiviruses.

摘要

为了研究猫免疫缺陷病毒和猴免疫缺陷病毒(分别为FIV和SIV)的基质(MA)蛋白之间的功能关系,我们构建了嵌合前病毒,其中SIV感染性分子克隆的MA编码区部分或全部被其FIV对应区域取代。含有FIV MA氨基末端36个残基或中央及羧基末端区域的嵌合SIV前病毒与野生型SIV一样有效地组装成病毒粒子。然而,在单循环感染性试验中,产生的病毒粒子没有感染性。此外,发现含有整个FIV MA的嵌合SIV前病毒由于嵌合Gag多蛋白的膜结合效率低下,在病毒粒子产生方面严重受损。有趣的是,这种嵌合Gag前体的组装缺陷表型可以通过在FIV衍生的MA结构域中引入G31K/G33K双氨基酸取代或与野生型SIV Gag共表达来逆转。值得注意的是,表达SIV MA的嵌合FIV前病毒不仅与野生型FIV一样有效地组装成颗粒,而且在猫T细胞中以野生型动力学进行复制。因此,我们的结果提供了关于远亲慢病毒MA蛋白之间功能同源性的新信息。

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