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Identification and Visualization of Functionally Important Domains and Residues in Herpes Simplex Virus Glycoprotein K(gK) Using a Combination of Phylogenetics and Protein Modeling

机译:使用系统发育和蛋白质建模的组合鉴定和可视化单纯疱疹病毒糖蛋白K(GK)中的功能重要结构型和残留物

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Alphaherpesviruses are a subfamily of herpesviruses that include the significant human pathogens herpes simplex viruses (HSV) and varicella zoster virus (VZV). Glycoprotein K (gK), conserved in all alphaherpesviruses, is a multi-membrane spanning virion glycoprotein essential for virus entry into neuronal axons, virion assembly, and pathogenesis. Despite these critical functions, little is known about which gK domains and residues are most important for maintaining these functions across all alphaherpesviruses. Herein, we employed phylogenetic and structural analyses including the use of a novel model for evolutionary rate variation across residues to predict conserved gK functional domains. We found marked heterogeneity in the evolutionary rate at the level of both individual residues and domains, presumably as a result of varying selective constraints. To clarify the potential role of conserved sequence features, we predicted the structures of several gK orthologs. Congruent with our phylogenetic analysis, slowly evolving residues were identified at potentially structurally significant positions across domains. We found that using a quantitative measure of amino acid rate variation combined with molecular modeling we were able to identify amino acids predicted to be critical for gK protein structure/function. This analysis yields targets for the design of anti-herpesvirus therapeutic strategies across all alphaherpesvirus species that would be absent from more traditional analyses of conservation.
机译:Alphaherpesviruses是疱疹病毒的亚家族,包括重要人类病原体疱疹病毒(HSV)和水痘带状疱疹病毒(VZV)。糖蛋白K(GK)保守所有αpesviruses,是一种多膜跨越病毒蛋白糖蛋白,其对于病毒进入神经元轴突,病毒群体组装和发病机构。尽管存在这些关键功能,但众所周知,在所有αherpesviruses上维持这些功能最重要的是。在此,我们使用系统发育和结构分析,包括使用新型模型以防止残留物的进化速率变化来预测保守的GK功能域。我们发现了在各个残留物和域的水平的进化率中发现了标记的异质性,这可能是由于不同选择性约束的结果。为了澄清保守序列特征的潜在作用,我们预测了几个GK Orthologs的结构。随着系统发育分析的一致性,在跨域潜在的结构上显着的位置鉴定缓慢不断发展的残留物。我们发现,使用氨基酸速率变化的定量测量与分子建模联合我们能够鉴定预测对GK蛋白质结构/功能至关重要的氨基酸。该分析产生了在所有alphaherpesvirus种类上设计抗herpesvirus治疗策略的靶标,这将不存在更传统的保护分析。

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