Polymorphisms of large effect explain the majority of the host genetic contribution to variation of HIV-1 virus load

Author:

McLaren Paul J.ORCID,Coulonges Cedric,Bartha István,Lenz Tobias L.,Deutsch Aaron J.,Bashirova Arman,Buchbinder Susan,Carrington Mary N.,Cossarizza Andrea,Dalmau Judith,De Luca Andrea,Goedert James J.,Gurdasani Deepti,Haas David W.,Herbeck Joshua T.,Johnson Eric O.,Kirk Gregory D.,Lambotte Olivier,Luo Ma,Mallal Simon,van Manen Daniëlle,Martinez-Picado Javier,Meyer Laurence,Miro José M.,Mullins James I.,Obel Niels,Poli Guido,Sandhu Manjinder S.,Schuitemaker Hanneke,Shea Patrick R.,Theodorou Ioannis,Walker Bruce D.,Weintrob Amy C.,Winkler Cheryl A.,Wolinsky Steven M.,Raychaudhuri Soumya,Goldstein David B.,Telenti Amalio,de Bakker Paul I. W.,Zagury Jean-François,Fellay Jacques

Abstract

Previous genome-wide association studies (GWAS) of HIV-1–infected populations have been underpowered to detect common variants with moderate impact on disease outcome and have not assessed the phenotypic variance explained by genome-wide additive effects. By combining the majority of available genome-wide genotyping data in HIV-infected populations, we tested for association between ∼8 million variants and viral load (HIV RNA copies per milliliter of plasma) in 6,315 individuals of European ancestry. The strongest signal of association was observed in the HLA class I region that was fully explained by independent effects mapping to five variable amino acid positions in the peptide binding grooves of the HLA-B and HLA-A proteins. We observed a second genome-wide significant association signal in the chemokine (C-C motif) receptor (CCR) gene cluster on chromosome 3. Conditional analysis showed that this signal could not be fully attributed to the known protective CCR5Δ32 allele and the risk P1 haplotype, suggesting further causal variants in this region. Heritability analysis demonstrated that common human genetic variation—mostly in the HLA and CCR5 regions—explains 25% of the variability in viral load. This study suggests that analyses in non-European populations and of variant classes not assessed by GWAS should be priorities for the field going forward.

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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