Sequence-based in silico analysis of well studied Hepatitis C Virus epitopes and their variants in other genotypes (particularly genotype 5a) against South African human leukocyte antigen backgrounds

dc.contributorBowyer, Sheila Mary
dc.contributor.authorPrabdial-Sing, Nishi
dc.contributor.authorPuren, Adrian
dc.contributor.authorBowyer, Sheila Mary
dc.date.accessioned2013-02-27T13:54:16Z
dc.date.available2013-02-27T13:54:16Z
dc.date.issued2012-12-10
dc.description.abstractBACKGROUND: Host genetics influence the outcome of HCV disease. HCV is also highly mutable and escapes host immunity. HCV genotypes are geographically distributed and HCV subtypes have been shown to have distinct repertoires of HLA-restricted viral epitopes which explains the lack of cross protection across genotypes observed in some studies. Despite this, immune databases and putative epitope vaccines concentrate almost exclusively on HCV genotype 1 class I-epitopes restricted by the HLA-A*02 allele. While both genotype and allele predominate in developed countries, we hypothesise that HCV variation and population genetics will affect the efficacy of proposed epitope vaccines in South Africa. This in silico study investigates HCV viral variability within well-studied epitopes identified in genotype 1 and uses algorithms to predict the immunogenicity of their variants from other less studied genotypes and thus rate the most promising vaccine candidates for the South African population. Six class I- and seven class II- restricted epitope sequences within the core, NS3, NS4B and NS5B regions were compared across the six HCV genotypes using local genotype 5a sequence data together with global data. Common HLA alleles in the South African population are A30:01, A02:01, B58:02, B07:02; DRB1*13:01 and DRB1*03:01. Epitope binding to 13 class I- and 8 class –II alleles were described using web-based prediction servers, Immune Epitope Database, (IEDB) and Propred. Online population coverage tools were used to assess vaccine efficacy. RESULTS: Despite the homogeneity of genotype 1 and genotype 5 over the epitopes, there was limited promiscuity to local HLA-alleles.Host differences will make a putative vaccine less effective in South Africa. Of the 6 well-characterized class I- epitopes, only 2 class I- epitopes were promiscuous and 3 of the 7 class-II epitopes were better conserved and promiscuous. By fine tuning the putative vaccine using an optimal cocktail of genotype 1 and 5a epitopes and local HLA data, the coverage was raised from 65.85% to 91.87% in South African Blacks. CONCLUSION: While in vivo and in vitro studies are needed to confirm immunogenic epitopes, in silico HCV epitope vaccine design which takes into account HCV variation and host allele frequency will maximize population coverage in different ethnic groups.en_US
dc.description.librarianam2013en_US
dc.description.librarianay2013en
dc.description.sponsorshipThe Poliomyelitis research foundation, PRF grant 07/17en_US
dc.description.urihttp://www.biomedcentral.com/1471-2172/13/67en_US
dc.identifier.citationPrabdial-Sing et al.: Sequence-based in silico analysis of well studied Hepatitis C Virus epitopes and their variants in other genotypes (particularly genotype 5a) against South African human leukocyte antigen backgrounds. BMC Immunology 2012 13:67.en_US
dc.identifier.issn1471-2172
dc.identifier.other10.1186/1471-2172-13-67
dc.identifier.urihttp://hdl.handle.net/2263/21151
dc.language.isoenen_US
dc.publisherBioMed Centralen_US
dc.rights© 2012 Prabdial-Sing et al.; licensee BioMed Central Ltd. This is an Open Access article distributed under the terms of the Creative Commons Attribution Licenseen_US
dc.subjectEpitope vaccinesen_US
dc.subjectViral variationen_US
dc.subjectPopulation coverageen_US
dc.subjectHLAen_US
dc.subjectEpitope predictionen_US
dc.subjectHepatitis C virus (HCV)en_US
dc.subject.lcshVaccination -- South Africaen
dc.titleSequence-based in silico analysis of well studied Hepatitis C Virus epitopes and their variants in other genotypes (particularly genotype 5a) against South African human leukocyte antigen backgroundsen_US
dc.typeArticleen_US

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