Prediction of promiscuous T-cell epitopes in the Zika virus polyprotein:An in silico approach

被引:0
|
作者
Hamza Dar [1 ]
Tahreem Zaheer [1 ]
Muhammad Talha Rehman [1 ]
Amjad Ali [1 ]
Aneela Javed [1 ]
Gohar Ayub Khan [1 ]
Mustafeez Mujtaba Babar [2 ]
Yasir Waheed [3 ]
机构
[1] Atta-ur-Rahman School of Applied Biosciences(ASAB),National University of Sciences and Technology
[2] Shifa College of Pharmaceutical Sciences,Shifa Tameer-e-Millat University  3. Foundation University Medical College,Foundation University Islamabad
关键词
Zika Virus; B-Cell Epitopes; T-Cell Epitopes; Vaccine; Antigenicity;
D O I
暂无
中图分类号
R392 [医学免疫学];
学科分类号
100102 ;
摘要
Objective:To predict immunogenic promiscuous T-cell epitopes from the polyprotein of the Zika virus using a range of bioinformatics tools.To date,no epitope data are available for the Zika virus in the IEDB database.Methods:We retrieved nearly 54 full length polyprotein sequences of the Zika virus from the NCBI database belonging to different outbreaks.A consensus sequence was then used to predict the promiscuous T cell epitopes that bind MHC 1 and MHC II alleles using Propred1 and Propred immunoinformatic algorithms respectively.The antigencity predicted score was also calculated for each predicted epitope using the Vaxi Jen 2.0 tool.Results:By using Pro Pred1,23 antigenic epitopes for HLA class I and 48 antigenic epitopes for HLA class II were predicted from the consensus polyprotein sequence of Zika virus.The greatest number of MHC class I binding epitopes were projected within the NS5(21%),followed by Envelope(17%).For MHC class II,greatest number of predicted epitopes were in NS5(19%) followed by the Envelope,NS1 and NS2(17% each).A variety of epitopes with good binding affinity,promiscuity and antigenicity were predicted for both the HLA classes.Conclusion:The predicted conserved promiscuous T-cell epitopes examined in this study were reported for the first time and will contribute to the imminent design of Zika virus vaccine candidates,which will be able to induce a broad range of immune responses in a heterogeneous HLA population.However,our results can be verified and employed in future efficacious vaccine formulations only after successful experimental studies.
引用
收藏
页码:822 / 828
页数:7
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