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首页> 外文期刊>Retrovirology >Computational analysis of envelope glycoproteins from diverse geographical isolates of bovine leukemia virus identifies highly conserved peptide motifs
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Computational analysis of envelope glycoproteins from diverse geographical isolates of bovine leukemia virus identifies highly conserved peptide motifs

机译:来自牛白血病病毒不同地理分离株的包膜糖蛋白的计算分析确定了高度保守的肽基序

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BackgroundBovine leukemia virus (BLV) is a deltaretrovirus infecting bovine B cells and causing enzootic bovine leucosis. The SU or surface subunit, gp51, of its envelope glycoprotein is involved in receptor recognition and virion attachment. It contains the major neutralizing and CD4+ and CD8+ T cell epitopes found in naturally infected animals. In this study, we aimed to determine global variation and conservation within gp51 in the context of developing an effective global BLV vaccine. ResultsA total of 256 sequences extracted from the NCBI database and collected in different parts of the world, were studied to identify conserved segments along the env gene sequences that encode the gp51 protein. Using the MEME server and the conserved DNA Region module for analysis within DnaSP, we identified six conserved segments, referred to as A–F, and five semi-conserved segments, referred to as G–K. The amino acid conservation ranged from 98.8 to 99.8% in conserved segments A to F, while segments G to K had 89.6–95.2% conserved amino acid sequence. Selection analysis of individual segments revealed that residues of conserved segments had undergone purifying selection, whereas, particular residues in the semi-conserved segments are currently undergoing positive selection, specifically at amino acid positions 48 in segment K, 74 in segment G, 82 in segment I, 133 and 142 in segment J, and residue 291 in segment H. Each of the codons for these six residues contain the most highly variable nucleotides within their respective semi-conserved segments. ConclusionsThe data described here show that the consensus amino acid sequence constitutes a strong candidate from which a global vaccine can be derived for use in countries where eradication by culling is not economically feasible. The most conserved segments overlap with amino acids in known immunodeterminants, specifically in epitopes D–D′, E-E′, CD8+ T-cell epitopes, neutralizing domain 1 and CD4+ T-cell epitopes. Two of the segments reported here represent unique segments that do not overlap with previously identified antigenic determinants. We propose that evidence of positive selection in some residues of the semi-conserved segments suggests that their variation is involved in viral strategy to escape immune surveillance of the host.
机译:背景牛白血病病毒(BLV)是一种三角型病毒,会感染牛B细胞并引起牛源性牛白血病。其包膜糖蛋白的SU或表面亚基gp51与受体识别和病毒体附着有关。它包含在自然感染的动物中发现的主要中和以及CD4 +和CD8 + T细胞表位。在这项研究中,我们旨在在开发有效的全球BLV疫苗的背景下确定gp51内的全球变异和保守性。结果研究了从NCBI数据库中提取并收集到世界不同地区的256个序列,以鉴定沿编码gp51蛋白的env基因序列的保守区段。使用MEME服务器和保守的DNA区域模块在DnaSP中进行分析,我们确定了六个保守的片段(称为A–F)和五个半保守的片段(称为GG)。保守区段A至F的氨基酸保守性范围为98.8至99.8%,而区段G至K的保守氨基酸序列为89.6–95.2%。对单个片段的选择分析显示,保守片段的残基已经过纯化选择,而半保守片段中的特定残基目前正进行正选择,特别是在片段K的氨基酸位置48,片段G的氨基酸74,片段的82片段J中的I,133和142,以及片段H中的残基291。这六个残基的每个密码子在其各自的半保守片段中均包含变化最大的核苷酸。结论此处描述的数据表明,共有氨基酸序列是很强的候选者,可以从中衍生出全球疫苗,用于在经济上不可行淘汰扑灭的国家。在已知的免疫决定簇中,最保守的片段与氨基酸重叠,特别是在表位D-D',E-E',CD8 + T细胞表位,中和域1和CD4 + T细胞表位中。此处报道的两个片段代表与先前鉴定的抗原决定簇不重叠的独特片段。我们建议在半保守区段的某些残基中进行阳性选择的证据表明,它们的变异参与了病毒策略以逃避宿主的免疫监视。

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