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泡沫病毒包膜糖蛋白的比较序列分析与预测

Comparative sequence analysis and predictions for the envelope glycoproteins of foamy viruses.

作者信息

Wang G, Mulligan M J

出版信息

J Gen Virol. 1999 Jan;80 ( Pt 1):245-254. doi: 10.1099/0022-1317-80-1-245.

Abstract

The foamy viruses (FVs) are a genus of complex retroviruses that has recently been found to possess several novel molecular features. There is increasing interest in the development of FVs as novel vectors for gene delivery. As there are remarkably few published studies of FV proteins, these recent findings prompted us to predict the structural features of FV glycoproteins with the aid of computer programs. We analysed all seven available FV Env sequences, a greater number of sequences than in previously published analyses. The relative rates of change for FV structural proteins were Pol < Env < Gag in increasing order, which differs from all other retroviruses. We determined that this difference is primarily caused by a higher relative rate of change for FV Gag proteins. We analysed the functional domains of FV glycoproteins and found that their structural organization was generally similar to other retroviruses. Putative structures were identified for the signal peptide, cleavage site, fusion peptide, membrane-spanning domain and the unique endoplasmic reticulum retrieval signal. Based on the predicted secondary structure of the transmembrane glycoprotein (TM) subunit, gp47, we also identified a unique prolonged central 'sheets and loops' region as the dominant feature of an unusually lengthy TM ectodomain. This lengthy central domain was flanked at each end by alpha-helices. The predictions reported here will stimulate and facilitate experimental approaches to better understand the structure and function of FV glycoproteins, and should assist in the planning and development of FV vectors.

摘要

泡沫病毒(FVs)是一类复杂的逆转录病毒,最近发现它们具有一些新的分子特征。人们对开发FVs作为新型基因递送载体的兴趣与日俱增。由于关于FV蛋白的已发表研究非常少,这些最新发现促使我们借助计算机程序预测FV糖蛋白的结构特征。我们分析了所有七个可用的FV Env序列,其数量比以前发表的分析中更多。FV结构蛋白的相对变化率按升序排列为Pol < Env < Gag,这与所有其他逆转录病毒不同。我们确定这种差异主要是由FV Gag蛋白较高的相对变化率引起的。我们分析了FV糖蛋白的功能域,发现它们的结构组织与其他逆转录病毒大致相似。确定了信号肽、切割位点、融合肽、跨膜结构域和独特的内质网回收信号的推定结构。基于跨膜糖蛋白(TM)亚基gp47的预测二级结构,我们还确定了一个独特的延长的中央“片层和环”区域,作为异常长的TM胞外域的主要特征。这个长的中央结构域两端各有一个α螺旋。本文报道的预测将激发并促进实验方法,以更好地理解FV糖蛋白的结构和功能,并应有助于FV载体的规划和开发。

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