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Computational elucidation of potential antigenic CTL epitopes in Ebola virus.

Authors :
Dikhit, Manas R.
Kumar, Santosh
Vijaymahantesh, null
Sahoo, Bikash R.
Mansuri, Rani
Amit, Ajay
Yousuf Ansari, Md.
Sahoo, Ganesh C.
Bimal, Sanjiva
Das, Pradeep
Source :
Infection, Genetics & Evolution. Dec2015, Vol. 36, p369-375. 7p.
Publication Year :
2015

Abstract

Cell-mediated immunity is important for the control of Ebola virus infection. We hypothesized that those HLA A0201 and HLA B40 restricted epitopes derived from Ebola virus proteins, would mount a good antigenic response. Here we employed an immunoinformatics approach to identify specific 9mer amino acid which may be capable of inducing a robust cell-mediated immune response in humans. We identified a set of 28 epitopes that had no homologs in humans. Specifically, the epitopes derived from NP, RdRp, GP and VP40 share population coverage of 93.40%, 84.15%, 74.94% and 77.12%, respectively. Based on the other HLA binding specificity and population coverage, seven novel promiscuous epitopes were identified. These 7 promiscuous epitopes from NP, RdRp and GP were found to have world-wide population coverage of more than 95% indicating their potential significance as useful candidates for vaccine design. Epitope conservancy analysis also suggested that most of the peptides are highly conserved (100%) in other virulent Ebola strain (Mayinga-76, Kikwit-95 and Makona-G3816- 2014) and can therefore be further investigated for their immunological relevance and usefulness as vaccine candidates. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
15671348
Volume :
36
Database :
Academic Search Index
Journal :
Infection, Genetics & Evolution
Publication Type :
Academic Journal
Accession number :
110855759
Full Text :
https://doi.org/10.1016/j.meegid.2015.10.012