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PVS: a web server for protein sequence variability analysis tuned to facilitate conserved epitope discovery

机译:PVS:用于蛋白质序列变异性分析的Web服务器经过调整可促进保守表位的发现

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摘要

We have developed PVS (Protein Variability Server), a web-based tool that uses several variability metrics to compute the absolute site variability in multiple protein-sequence alignments (MSAs). The variability is then assigned to a user-selected reference sequence consisting of either the first sequence in the alignment or a consensus sequence. Subsequently, PVS performs tasks that are relevant for structure-function studies, such as plotting and visualizing the variability in a relevant 3D-structure. Neatly, PVS also implements some other tasks that are thought to facilitate the design of epitope discovery-driven vaccines against pathogens where sequence variability largely contributes to immune evasion. Thus, PVS can return the conserved fragments in the MSA—as defined by a user-provided variability threshold—and locate them in a relevant 3D-structure. Furthermore, PVS can return a variability-masked sequence, which can be directly submitted to the RANKPEP server for the prediction of conserved T-cell epitopes. PVS is freely available at: .
机译:我们已经开发了PVS(蛋白质变异性服务器),这是一个基于Web的工具,它使用多种变异性指标来计算多个蛋白质序列比对(MSA)中的绝对位点变异性。然后将变异性分配给用户选择的参考序列,该序列由比对中的第一个序列或共有序列组成。随后,PVS执行与结构功能研究相关的任务,例如绘制和可视化相关3D结构中的变异性。整洁地,PVS还执行其他一些任务,这些任务被认为可以促进针对病原体的表位发现驱动的疫苗的设计,这些病原体的序列变异性在很大程度上有助于逃避免疫。因此,PVS可以将MSA中的保守片段(由用户提供的可变性阈值定义)返回,并将其定位在相关的3D结构中。此外,PVS可以返回变异性屏蔽的序列,该序列可以直接提交给RANKPEP服务器以预测保守的T细胞表位。 PVS可在以下位置免费获得。

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