Genome-wide mRNA expression correlates of viral control in CD4+ T-cells from HIV-1-infected individuals.

There is great interindividual variability in HIV-1 viral setpoint after seroconversion, some of which is known to be due to genetic differences among infected individuals. Here, our focus is on determining, genome-wide, the contribution of variable gene expression to viral control, and to relate it...

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Main Authors: Margalida Rotger, Kristen K Dang, Jacques Fellay, Erin L Heinzen, Sheng Feng, Patrick Descombes, Kevin V Shianna, Dongliang Ge, Huldrych F Günthard, David B Goldstein, Amalio Telenti, Swiss HIV Cohort Study, Center for HIV/AIDS Vaccine Immunology
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2010-02-01
Series:PLoS Pathogens
Online Access:http://europepmc.org/articles/PMC2829051?pdf=render
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spelling doaj-70b9ed040f53413f865b468509610dbd2020-11-25T01:47:10ZengPublic Library of Science (PLoS)PLoS Pathogens1553-73661553-73742010-02-0162e100078110.1371/journal.ppat.1000781Genome-wide mRNA expression correlates of viral control in CD4+ T-cells from HIV-1-infected individuals.Margalida RotgerKristen K DangJacques FellayErin L HeinzenSheng FengPatrick DescombesKevin V ShiannaDongliang GeHuldrych F GünthardDavid B GoldsteinAmalio TelentiSwiss HIV Cohort StudyCenter for HIV/AIDS Vaccine ImmunologyThere is great interindividual variability in HIV-1 viral setpoint after seroconversion, some of which is known to be due to genetic differences among infected individuals. Here, our focus is on determining, genome-wide, the contribution of variable gene expression to viral control, and to relate it to genomic DNA polymorphism. RNA was extracted from purified CD4+ T-cells from 137 HIV-1 seroconverters, 16 elite controllers, and 3 healthy blood donors. Expression levels of more than 48,000 mRNA transcripts were assessed by the Human-6 v3 Expression BeadChips (Illumina). Genome-wide SNP data was generated from genomic DNA using the HumanHap550 Genotyping BeadChip (Illumina). We observed two distinct profiles with 260 genes differentially expressed depending on HIV-1 viral load. There was significant upregulation of expression of interferon stimulated genes with increasing viral load, including genes of the intrinsic antiretroviral defense. Upon successful antiretroviral treatment, the transcriptome profile of previously viremic individuals reverted to a pattern comparable to that of elite controllers and of uninfected individuals. Genome-wide evaluation of cis-acting SNPs identified genetic variants modulating expression of 190 genes. Those were compared to the genes whose expression was found associated with viral load: expression of one interferon stimulated gene, OAS1, was found to be regulated by a SNP (rs3177979, p = 4.9E-12); however, we could not detect an independent association of the SNP with viral setpoint. Thus, this study represents an attempt to integrate genome-wide SNP signals with genome-wide expression profiles in the search for biological correlates of HIV-1 control. It underscores the paradox of the association between increasing levels of viral load and greater expression of antiviral defense pathways. It also shows that elite controllers do not have a fully distinctive mRNA expression pattern in CD4+ T cells. Overall, changes in global RNA expression reflect responses to viral replication rather than a mechanism that might explain viral control.http://europepmc.org/articles/PMC2829051?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Margalida Rotger
Kristen K Dang
Jacques Fellay
Erin L Heinzen
Sheng Feng
Patrick Descombes
Kevin V Shianna
Dongliang Ge
Huldrych F Günthard
David B Goldstein
Amalio Telenti
Swiss HIV Cohort Study
Center for HIV/AIDS Vaccine Immunology
spellingShingle Margalida Rotger
Kristen K Dang
Jacques Fellay
Erin L Heinzen
Sheng Feng
Patrick Descombes
Kevin V Shianna
Dongliang Ge
Huldrych F Günthard
David B Goldstein
Amalio Telenti
Swiss HIV Cohort Study
Center for HIV/AIDS Vaccine Immunology
Genome-wide mRNA expression correlates of viral control in CD4+ T-cells from HIV-1-infected individuals.
PLoS Pathogens
author_facet Margalida Rotger
Kristen K Dang
Jacques Fellay
Erin L Heinzen
Sheng Feng
Patrick Descombes
Kevin V Shianna
Dongliang Ge
Huldrych F Günthard
David B Goldstein
Amalio Telenti
Swiss HIV Cohort Study
Center for HIV/AIDS Vaccine Immunology
author_sort Margalida Rotger
title Genome-wide mRNA expression correlates of viral control in CD4+ T-cells from HIV-1-infected individuals.
title_short Genome-wide mRNA expression correlates of viral control in CD4+ T-cells from HIV-1-infected individuals.
title_full Genome-wide mRNA expression correlates of viral control in CD4+ T-cells from HIV-1-infected individuals.
title_fullStr Genome-wide mRNA expression correlates of viral control in CD4+ T-cells from HIV-1-infected individuals.
title_full_unstemmed Genome-wide mRNA expression correlates of viral control in CD4+ T-cells from HIV-1-infected individuals.
title_sort genome-wide mrna expression correlates of viral control in cd4+ t-cells from hiv-1-infected individuals.
publisher Public Library of Science (PLoS)
series PLoS Pathogens
issn 1553-7366
1553-7374
publishDate 2010-02-01
description There is great interindividual variability in HIV-1 viral setpoint after seroconversion, some of which is known to be due to genetic differences among infected individuals. Here, our focus is on determining, genome-wide, the contribution of variable gene expression to viral control, and to relate it to genomic DNA polymorphism. RNA was extracted from purified CD4+ T-cells from 137 HIV-1 seroconverters, 16 elite controllers, and 3 healthy blood donors. Expression levels of more than 48,000 mRNA transcripts were assessed by the Human-6 v3 Expression BeadChips (Illumina). Genome-wide SNP data was generated from genomic DNA using the HumanHap550 Genotyping BeadChip (Illumina). We observed two distinct profiles with 260 genes differentially expressed depending on HIV-1 viral load. There was significant upregulation of expression of interferon stimulated genes with increasing viral load, including genes of the intrinsic antiretroviral defense. Upon successful antiretroviral treatment, the transcriptome profile of previously viremic individuals reverted to a pattern comparable to that of elite controllers and of uninfected individuals. Genome-wide evaluation of cis-acting SNPs identified genetic variants modulating expression of 190 genes. Those were compared to the genes whose expression was found associated with viral load: expression of one interferon stimulated gene, OAS1, was found to be regulated by a SNP (rs3177979, p = 4.9E-12); however, we could not detect an independent association of the SNP with viral setpoint. Thus, this study represents an attempt to integrate genome-wide SNP signals with genome-wide expression profiles in the search for biological correlates of HIV-1 control. It underscores the paradox of the association between increasing levels of viral load and greater expression of antiviral defense pathways. It also shows that elite controllers do not have a fully distinctive mRNA expression pattern in CD4+ T cells. Overall, changes in global RNA expression reflect responses to viral replication rather than a mechanism that might explain viral control.
url http://europepmc.org/articles/PMC2829051?pdf=render
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