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牛免疫缺陷病毒中糖蛋白45跨膜结构域的鉴定

Identification of the membrane-spanning domain of glycoprotein 45 in bovine immunodeficiency virus.

作者信息

Shen W, Feng J, Liu Z, Diao D, Liu C H, Kong X

出版信息

Acta Virol. 2018;62(3):294-303. doi: 10.4149/av_2018_223.

Abstract

The membrane-spanning domain (MSD) of the transmembrane subunit (TM) anchors the envelope glycoprotein (Env) on the lipid bilayer of the host cell membrane and virions. Its functions include membrane fusion efficiency and intracellular trafficking of the lentivirus envelope protein. Our study aimed to determine the MSD of bovine immunodeficiency virus (BIV) glycoprotein 45 (gp45) and reveal structural characteristics of the BIV Env protein. We have predicted the region of the BIV MSD and obtained the sequence using bioinformatics software. Various kinds of assays, including analogy analysis, fluorescence microscopy, and dye-transfer-based assays, were carried out to validate the prediction. The results, for the first time, show that the BIV MSD is located at the D170 to M191 amino acids of gp45, and the identified MSD divides gp45 into the extracellular domain (ED), MSD and cytoplasmic domain (CT). We further found that the BIV MSD had a similar structure and function as the HIV MSD using amino acid sequence alignment and fluorescence microscopy. Additionally, the dye-transfer-based assay demonstrates that deletion of the BIV MSD efficiently decreases cell-cell fusion. Based on the identification of the MSD, a "snorkeling" model, in which the flanking charged amino acid residues are buried in the lipid bilayer while their side chains interact with polar head groups, was proposed for the BIV MSD. Ultimately, we further improved the primary structure of the BIV envelope glycoprotein.

摘要

跨膜亚基(TM)的跨膜结构域(MSD)将包膜糖蛋白(Env)锚定在宿主细胞膜和病毒体的脂质双层上。其功能包括膜融合效率和慢病毒包膜蛋白的细胞内运输。我们的研究旨在确定牛免疫缺陷病毒(BIV)糖蛋白45(gp45)的MSD,并揭示BIV Env蛋白的结构特征。我们已经预测了BIV MSD的区域,并使用生物信息学软件获得了序列。进行了各种分析,包括类比分析、荧光显微镜检查和基于染料转移的分析,以验证预测结果。结果首次表明,BIV MSD位于gp45的第170至191个氨基酸处,所确定的MSD将gp45分为细胞外结构域(ED)、MSD和细胞质结构域(CT)。我们进一步发现,使用氨基酸序列比对和荧光显微镜检查,BIV MSD与HIV MSD具有相似的结构和功能。此外,基于染料转移的分析表明,缺失BIV MSD可有效降低细胞间融合。基于对MSD的鉴定,我们为BIV MSD提出了一种“潜水”模型,即侧翼带电荷的氨基酸残基埋在脂质双层中,而它们的侧链与极性头部基团相互作用。最终,我们进一步完善了BIV包膜糖蛋白的一级结构。

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