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In silico identification of common epitopes from pathogenic mycobacteria

机译:在计算机上鉴定致病性分枝杆菌的常见表位

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An in silico study was carried out to identify antigens for their possible collective use as vaccine candidates against diseases caused by different classes of pathogenic mycobacteria with significant clinical relevance. The genome sequences of the relevant causative agents were used in order to search for orthologous genes among them. Bioinformatics tools permitted us to identify several conserved sequences with 100% identity with no possibility of cross-reactivity to the normal flora and human proteins. Nine different proteins were characterized using the strain H37Rv as reference and taking into account their functional category, their in vivo expression and subcellular location. T and B cell epitopes were identified in the selected sequences. Theoretical prediction of population coverage was calculated for individual epitopes as well as their combinations. Several identical sequences, belonging to six proteins containing T and B cell epitopes which are not present in selected microorganisms of the normal microbial flora or in human proteins were obtained.
机译:进行了一项计算机研究,以鉴定抗原作为可能的候选疫苗,以对抗由不同种类的致病性分枝杆菌引起的疾病,具有重要的临床意义。为了寻找其中的直系同源基因,使用了相关病原体的基因组序列。生物信息学工具使我们能够鉴定出几个具有100%同一性的保守序列,而不会与正常菌群和人类蛋白质发生交叉反应。使用菌株H37Rv作为参考,并考虑到它们的功能类别,它们的体内表达和亚细胞位置,表征了9种不同的蛋白。在选择的序列中鉴定出T和B细胞表位。计算单个表位及其组合的人口覆盖率的理论预测。获得了属于六个含有T和B细胞表位的蛋白质的几个相同序列,这些蛋白质在正常微生物菌群的选定微生物或人蛋白质中不存在。

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