预测埃博拉病毒候选表位，用于可能的疫苗开发

2015 IEEE/ACM International Conference on Advances in Social Networks Analysis and Mining (ASONAM) Pub Date : 2015-08-25 DOI:10.1145/2808797.2809370

E. Raoufi, M. Hemmati, Hossein EinAbadi, H. Fallahi

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引用次数: 7

摘要

扎伊尔埃博拉病毒是丝状病毒科的一员，是引起出血热的原因。由于缺乏适当的抗病毒药物或疫苗，该病具有很强的致死率。在这项研究中，我们试图利用计算机方法和免疫信息学方法寻找扎伊尔埃博拉病毒(对MHC I、II和B细胞具有高抗原性)的浅表糖蛋白的表位。通过使用CTLPred, SYFPEITHI和Propred web应用程序用于MHC I类和SYFPEITHI和Propred1web应用程序用于MHC II类，我们已经能够找到得分最高的表位(肽)。此外，还使用了ElliPro、IgPred和Discotope网络工具来预测B细胞表位。选择序列“SRFTPQFLL”和“IFFLYDRLAS”作为MHCs分子的表位。选取255 ~ 310区域作为B细胞表位。预期这些多肽可以刺激免疫反应，用于设计抗ZEV多肽疫苗，但这些结果需要通过实验分析来证实。

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Predicting candidate epitopes on Ebolaviruse for possible vaccine development

Zaire ebolavirus a member of family Filoviridae is the cause of hemorrhagic fever. Due to lack of appropriate anti-viral or vaccine, this disease is very lethal. In this study we tried to find epitopes for superficial glycoprotein of Zaire ebolavirus (that have high antigenicity for MHC I, II and B cells) with use of in-silico methods and immunoinformatics approach. By use of CTLPred, SYFPEITHI and Propred web applications for MHC class I and SYFPEITHI and Propred1web applications for MHC class II we had been able to find epitopes (peptides) that have highest score. Also ElliPro, IgPred and Discotope web tools had been performed to predict B cells epitopes. The sequence "SRFTPQFLL" and "IFFLYDRLAS" were selected to be epitopes for MHCs molecules. The region 255 to 310 was selected for B cell epitope. It was expected these peptides could be stimulated immune response and used for designing multi-peptide vaccine against ZEV but these results should be reliable with experimental analysis.

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2015 IEEE/ACM International Conference on Advances in Social Networks Analysis and Mining (ASONAM)

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