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丙型肝炎病毒包膜糖蛋白的互补模式以及胞外和跨膜结构域的作用。

Hepatitis C virus envelope glycoproteins complementation patterns and the role of the ecto- and transmembrane domains.

作者信息

Lin Xiaojing, Zhang Yonghui, Bi Shengli, Lu Jian, Zhao Honglan, Tan Wenjie, Li Dexin, Wang Yue

机构信息

State Key Laboratory for Molecular Virology and Genetic Engineering, National Institute for Viral Disease Control and Prevention, Chinese Center for Disease Control and Prevention, Xuanwu District, Beijing, People's Republic of China.

出版信息

Biochem Biophys Res Commun. 2009 Jul 24;385(2):257-62. doi: 10.1016/j.bbrc.2009.05.068. Epub 2009 May 21.

Abstract

We separated E1 and E2 of hepatitis C virus (HCV) genotypes 1a, 1b, and 2a into two individual expression plasmids and replaced the transmembrane domains of 1b and 2a E1 and E2 with that of genotype 1a. The complementation features of E1 and E2 as well as the contributions of both the ecto- and transmembrane domains to the formation of the E1E2 complex were evaluated using the HCV pseudoparticle(s) (HCVpp(s)) system. We demonstrated that 1aE2 could not only complement its native 1aE1, but could also complement 1bE1 as well; in genotype 1b, glycoprotein complex formation is primarily dependent on the overall biological characteristics of the intact native E1 and E2; in genotype 2a, although the interaction of intact native E1 and E2 is critical for the formation of the glycoprotein complex, the ectodomain made a greater contribution than that of the transmembrane domain. Our study provides valuable findings regarding HCV E1 and E2 biology and will be of use in both anti-HCV strategy and understanding on the mechanisms of coinfection of different HCV strains.

摘要

我们将丙型肝炎病毒(HCV)1a、1b和2a基因型的E1和E2分别克隆到两个独立的表达质粒中,并将1b和2a基因型E1和E2的跨膜结构域替换为1a基因型的跨膜结构域。利用HCV假病毒颗粒(HCVpp)系统评估了E1和E2的互补特性,以及胞外结构域和跨膜结构域对E1E2复合物形成的贡献。我们证明,1aE2不仅可以与其天然的1aE1互补,还可以与1bE1互补;在1b基因型中,糖蛋白复合物的形成主要取决于完整天然E1和E2的整体生物学特性;在2a基因型中,虽然完整天然E1和E2的相互作用对糖蛋白复合物的形成至关重要,但胞外结构域比跨膜结构域的贡献更大。我们的研究为HCV E1和E2生物学提供了有价值的发现,将有助于抗HCV策略的制定以及对不同HCV毒株合并感染机制的理解。

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