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C6/36细胞浓核病毒的截短病毒样颗粒:对短浓核病毒组装机制的启示

The truncated virus-like particles of C6/36 cell densovirus: implications for the assembly mechanism of brevidensovirus.

作者信息

Li Zhihong, He Jian, Huang Xiaojun, Dai Aguang, Cheng Lingpeng, Shao Dingyong, Zhang Jingqiang

机构信息

Sun Yat-sen University, Guangzhou 510275, People's Republic of China.

出版信息

Virus Res. 2008 Mar;132(1-2):248-52. doi: 10.1016/j.virusres.2007.12.002. Epub 2008 Jan 16.

Abstract

The brevidensovirus is one of the smallest viruses in the world and the capsid of Aedes albopictus C6/36 cell densovirus (C6/36DNV) is the simplest and most compact capsid in brevidensovirus. To understand the assembly mechanism of icosahedral-virus capsid from this simplest model, we tried to express various lengths of virus proteins (VPs) of C6/36DNV in Bac-to-Bac system and evaluate their self-assembly capacities in insect Spodoptera frugiperda 9 (Sf9) cells. The result showed that the N-terminal GGSG sequence (residue 23-26), highly conserved glycine-rich region in Parvoviridae, and C-terminal GTGGVVTCMP (residue 344-353) were essential for capsid assembly, while the N-terminal nuclear localization signal, GTKRKR sequence (residue 15-20), was nonessential for the virus-like particles (VLPs) assembly, but did effect the formation of crystalline arrays in infected Sf9 cells. These information provided clues for how icosahedral-virus capsids formed and showed the potential of C6/36DNV-VLPs becoming a powerful nanoparticle vector.

摘要

短浓病毒是世界上最小的病毒之一,白纹伊蚊C6/36细胞浓病毒(C6/36DNV)的衣壳是短浓病毒中最简单、最紧凑的衣壳。为了从这个最简单的模型了解二十面体病毒衣壳的组装机制,我们尝试在杆状病毒表达系统中表达不同长度的C6/36DNV病毒蛋白(VPs),并在昆虫草地贪夜蛾9(Sf9)细胞中评估它们的自组装能力。结果表明,N端的GGSG序列(第23 - 26位氨基酸残基),这是细小病毒科中高度保守的富含甘氨酸区域,以及C端的GTGGVVTCMP(第344 - 353位氨基酸残基)对衣壳组装至关重要,而N端的核定位信号GTKRKR序列(第15 - 20位氨基酸残基)对病毒样颗粒(VLPs)的组装并非必需,但确实影响了感染的Sf9细胞中晶体阵列的形成。这些信息为二十面体病毒衣壳的形成方式提供了线索,并显示了C6/36DNV - VLPs成为一种强大的纳米颗粒载体的潜力。

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