Conference presentation
Relationship between HLA class I-driven evolution in Gag, Pol and Nef and clinical markers of HIV disease: A multi-center collaborative study
AIDS Vaccine 2008 (Cape Town, South Africa, 13/10/2008–16/10/2008)
2008
Abstract
Background: The relationship between immune escape and HIV disease is incompletely understood. Here we examine the relationship between CTL selection pressure and plasma viral load (pVL) by defining HLA class I-associated polymorphisms in Gag, Pol and Nef in a large cohort of untreated HIV-1 subtype B-infected persons.
Methods: HLA-associated polymorphisms were identified in >1200 chronically-infected, treatment-naïve individuals from Canada (HOMER cohort), the USA (ACTG5142/5128 protocols), and Western Australia (WAHC), using phylogenetically-corrected analysis methods incorporating a multivariate adjustment for HLA linkage disequilibrium and a q-value correction for multiple tests. In individuals for whom clinical data were available (N~550), correlations between pVL and HLA-associated polymorphisms were assessed using Spearman’s rank test.
Results: >1000 unique HLA-associated polymorphisms were identified, but the number of codons involved varied by protein: 22%, 16% and 48% of Gag, Pol and Nef codons harbored an HLA-associated polymorphism. Roughly 60% of polymorphisms mapped in or near known or predicted CTL epitopes; a further 20% likely represent compensatory mutations. A modest inverse correlation was observed between the total number of HLA-associated sites in Gag (but not Pol/Nef) and pVL (R=-0.13;p=0.002), suggesting that Gag CTL targeting contributes more substantially to viremia control than targeting other proteins. A positive correlation was observed between the proportion of escaped Gag (but not Pol/Nef) sites and pVL (R=0.11;p=0.01), suggesting that the consequences of escape in Gag may be greater than other proteins.
Conclusion: Results support strong CTL-mediated selection on HIV, the effects of which vary by protein. The list of >1000 HLA-associated polymorphisms represents the most comprehensive to date for HIV-subtype-B. The associations between pVL and CTL selection pressure/escape in Gag suggest that in vivo CTL targeting of Gag may be important clinically. These data have implications for HIV vaccines.
Details
- Title
- Relationship between HLA class I-driven evolution in Gag, Pol and Nef and clinical markers of HIV disease: A multi-center collaborative study
- Authors/Creators
- Z.L. Brumme (Author/Creator)M. John (Author/Creator)C.J. Brumme (Author/Creator)J.M. Carlson (Author/Creator)R. Haubrich (Author/Creator)S. Riddler (Author/Creator)L. Swenson (Author/Creator)I. Tao (Author/Creator)S. Szeto (Author/Creator)D. Chan (Author/Creator)C. Kadie (Author/Creator)N. Frahm (Author/Creator)C. Brander (Author/Creator)B. Walker (Author/Creator)D. Heckerman (Author/Creator)P.R. Harrigan (Author/Creator)S. Mallal (Author/Creator)
- Conference
- AIDS Vaccine 2008 (Cape Town, South Africa, 13/10/2008–16/10/2008)
- Identifiers
- 991005542557107891
- Murdoch Affiliation
- Centre for Clinical Immunology and Biomedical Statistics
- Language
- English
- Resource Type
- Conference presentation
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