Epitope Mapping of HIV-Specific CD8+ T cells in a Cohort Dominated by Clade A1 Infection
Date
2009Author
McKinnon, Lyle R
Mao, Xiaojuan
Kimani, Joshua
Wachihi, Charles
Semeniuk, Christina
Mendoza, Mark
Liang, Binhua
Luo, Ma
Fowke, Keith R
Plummer, Francis A
Ball, Blake T
Type
ArticleLanguage
enMetadata
Show full item recordAbstract
Background
CD8+ T cell responses are often detected at large magnitudes in HIV-infected subjects, and eliciting these responses is the central aim of many HIV-1 vaccine strategies. Population differences in CD8+ T cell epitope specificity will need to be understood if vaccines are to be effective in multiple geographic regions.
Methodology/Principal Findings
In a large Kenyan cohort, we compared responsive CD8+ T cell HIV-1 Env overlapping peptides (OLPs) to Best Defined Epitopes (BDEs), many of which have been defined in clade B infection. While the majority of BDEs (69%) were recognized in this population, nearly half of responsive OLPs (47%) did not contain described epitopes. Recognition frequencies of BDEs were inversely correlated to epitopic sequence differences between clade A1 and BDE (P = 0.019), and positively selected residues were more frequent in “new” OLPs (without BDEs). We assessed the impact of HLA and TAP binding on epitope recognition frequencies, focusing on predicted and actual epitopes in the HLA B7 supertype.
Conclusions/Significance
Although many previously described CD8 epitopes were recognized, several novel CD8 epitopes were defined in this population, implying that epitope mapping efforts have not been completely exhausted. Expansion of these studies will be critical to understand population differences in CD8 epitope recognition.
Citation
PLoS One. 2009; 4(9): e6965.Publisher
Department of Medical Microbiology
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Collections
- Faculty of Health Sciences (FHS) [10377]