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马尔堡病毒株糖蛋白基因和VP35基因的变异

Variation in the glycoprotein and VP35 genes of Marburg virus strains.

作者信息

Sanchez A, Trappier S G, Ströher U, Nichol S T, Bowen M D, Feldmann H

机构信息

Special Pathogens Branch, National Center for Infectious Diseases, Centers for Disease Control and Prevention, Atlanta, Georgia, USA.

出版信息

Virology. 1998 Jan 5;240(1):138-46. doi: 10.1006/viro.1997.8902.

Abstract

Marburg virus, the prototype of the family Filoviridae, differs genetically, serologically, and morphologically from Ebola viruses. To better define the genetic variation within the species, VP35 and glycoprotein (GP) genes of representative human isolates from four known episodes of Marburg virus hemorrhagic fever were analyzed. The percentage nucleotide differences in the GP gene coding regions of Marburg viruses (0.1-21%) was nearly equal to the percentage amino acid changes (0-23%), while the percentage nucleotide differences in VP35 coding regions (0.3-20.9%) were higher than the percentage amino acid changes (0.9-6.1%), indicating a greater number of nonsynonymous changes occurring in the GP gene. The higher variation in the GP gene and the corresponding protein, especially those changes in the variable middle region of the GP, suggests that the variability may be the result of responses to natural host pressures. Analysis of the GP gene open reading frame shows a nonrandom distribution of nonsynonymous mutations that may indicate positive Darwinian selection is operating within the variable region. A heptad repeat region and an adjoining predicted fusion peptide are found in the C-terminal third of Marburg virus GPs, as has been previously shown for Ebola virus, and are similar to those found in transmembrane glycoproteins of retroviruses, paramyxoviruses, coronaviruses, and influenza viruses. Comparative analyses showed that there are two lineages within the Marburg virus species of filoviruses. The most recent isolate from Kenya (1987) represents a separate genetic lineage within the Marburg virus species (21-23% amino acid difference). However, this lineage likely does not represent a separate Marburg subtype, as the extent of divergence is less than that separating Ebola virus subtypes.

摘要

马尔堡病毒是丝状病毒科的原型,在基因、血清学和形态学上与埃博拉病毒不同。为了更好地界定该物种内的基因变异情况,对来自马尔堡病毒出血热已知的4起疫情中的代表性人类分离株的VP35和糖蛋白(GP)基因进行了分析。马尔堡病毒GP基因编码区的核苷酸差异百分比(0.1% - 21%)与氨基酸变化百分比(0% - 23%)几乎相等,而VP35编码区的核苷酸差异百分比(0.3% - 20.9%)高于氨基酸变化百分比(0.9% - 6.1%),这表明GP基因中发生了更多的非同义变化。GP基因及其相应蛋白质的变异程度更高,尤其是GP可变中间区域的那些变化,这表明这种变异性可能是对自然宿主压力作出反应的结果。对GP基因开放阅读框的分析显示非同义突变呈非随机分布,这可能表明在可变区域内存在正向达尔文选择。正如之前在埃博拉病毒中所显示的那样,在马尔堡病毒GP的C端三分之一区域发现了一个七肽重复区域和一个相邻的预测融合肽,并且它们与在逆转录病毒、副粘病毒、冠状病毒和流感病毒的跨膜糖蛋白中发现的类似。比较分析表明,丝状病毒科的马尔堡病毒物种内存在两个谱系。来自肯尼亚的最新分离株(1987年)代表了马尔堡病毒物种内一个独立的遗传谱系(氨基酸差异为21% - 23%)。然而,这个谱系可能并不代表一个单独的马尔堡病毒亚型,因为其分化程度小于区分埃博拉病毒亚型的程度。

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