Association of TLR7 variants with AIDS-like disease and AIDS vaccine efficacy in rhesus macaques.

In HIV infection, TLR7-triggered IFN-α production exerts a direct antiviral effect through the inhibition of viral replication, but may also be involved in immune pathogenesis leading to AIDS. TLR7 could also be an important mediator of vaccine efficacy. In this study, we analyzed polymorphisms in t...

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Main Authors: Roman A Siddiqui, Michael Krawczak, Matthias Platzer, Ulrike Sauermann
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2011-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3192768?pdf=render
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spelling doaj-0f02d3f78496461084ee66b1584f87092020-11-25T01:42:29ZengPublic Library of Science (PLoS)PLoS ONE1932-62032011-01-01610e2547410.1371/journal.pone.0025474Association of TLR7 variants with AIDS-like disease and AIDS vaccine efficacy in rhesus macaques.Roman A SiddiquiMichael KrawczakMatthias PlatzerUlrike SauermannIn HIV infection, TLR7-triggered IFN-α production exerts a direct antiviral effect through the inhibition of viral replication, but may also be involved in immune pathogenesis leading to AIDS. TLR7 could also be an important mediator of vaccine efficacy. In this study, we analyzed polymorphisms in the X-linked TLR7 gene in the rhesus macaque model of AIDS. Upon resequencing of the TLR7 gene in 36 rhesus macaques of Indian origin, 12 polymorphic sites were detected. Next, we identified three tightly linked single nucleotide polymorphisms (SNP) as being associated with survival time. Genotyping of 119 untreated, simian immunodeficiency virus (SIV)-infected male rhesus macaques, including an 'MHC adjusted' subset, revealed that the three TLR7 SNPs are also significantly associated with set-point viral load. Surprisingly, this effect was not observed in 72 immunized SIV-infected male monkeys. We hypothesize (i) that SNP c.13G>A in the leader peptide is causative for the observed genotype-phenotype association and that (ii) the underlying mechanism is related to RNA secondary structure formation. Therefore, we investigated a fourth SNP (c.-17C>T), located 17 bp upstream of the ATG translation initiation codon, that is also potentially capable of influencing RNA structure. In c.13A carriers, neither set-point viral load nor survival time were related to the c.-17C>T genotype. In c.13G carriers, by contrast, the c.-17C allele was significantly associated with prolonged survival. Again, no such association was detected among immunized SIV-infected macaques. Our results highlight the dual role of TLR7 in immunodeficiency virus infection and vaccination and imply that it may be important to control human AIDS vaccine trials, not only for MHC genotype, but also for TLR7 genotype.http://europepmc.org/articles/PMC3192768?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Roman A Siddiqui
Michael Krawczak
Matthias Platzer
Ulrike Sauermann
spellingShingle Roman A Siddiqui
Michael Krawczak
Matthias Platzer
Ulrike Sauermann
Association of TLR7 variants with AIDS-like disease and AIDS vaccine efficacy in rhesus macaques.
PLoS ONE
author_facet Roman A Siddiqui
Michael Krawczak
Matthias Platzer
Ulrike Sauermann
author_sort Roman A Siddiqui
title Association of TLR7 variants with AIDS-like disease and AIDS vaccine efficacy in rhesus macaques.
title_short Association of TLR7 variants with AIDS-like disease and AIDS vaccine efficacy in rhesus macaques.
title_full Association of TLR7 variants with AIDS-like disease and AIDS vaccine efficacy in rhesus macaques.
title_fullStr Association of TLR7 variants with AIDS-like disease and AIDS vaccine efficacy in rhesus macaques.
title_full_unstemmed Association of TLR7 variants with AIDS-like disease and AIDS vaccine efficacy in rhesus macaques.
title_sort association of tlr7 variants with aids-like disease and aids vaccine efficacy in rhesus macaques.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2011-01-01
description In HIV infection, TLR7-triggered IFN-α production exerts a direct antiviral effect through the inhibition of viral replication, but may also be involved in immune pathogenesis leading to AIDS. TLR7 could also be an important mediator of vaccine efficacy. In this study, we analyzed polymorphisms in the X-linked TLR7 gene in the rhesus macaque model of AIDS. Upon resequencing of the TLR7 gene in 36 rhesus macaques of Indian origin, 12 polymorphic sites were detected. Next, we identified three tightly linked single nucleotide polymorphisms (SNP) as being associated with survival time. Genotyping of 119 untreated, simian immunodeficiency virus (SIV)-infected male rhesus macaques, including an 'MHC adjusted' subset, revealed that the three TLR7 SNPs are also significantly associated with set-point viral load. Surprisingly, this effect was not observed in 72 immunized SIV-infected male monkeys. We hypothesize (i) that SNP c.13G>A in the leader peptide is causative for the observed genotype-phenotype association and that (ii) the underlying mechanism is related to RNA secondary structure formation. Therefore, we investigated a fourth SNP (c.-17C>T), located 17 bp upstream of the ATG translation initiation codon, that is also potentially capable of influencing RNA structure. In c.13A carriers, neither set-point viral load nor survival time were related to the c.-17C>T genotype. In c.13G carriers, by contrast, the c.-17C allele was significantly associated with prolonged survival. Again, no such association was detected among immunized SIV-infected macaques. Our results highlight the dual role of TLR7 in immunodeficiency virus infection and vaccination and imply that it may be important to control human AIDS vaccine trials, not only for MHC genotype, but also for TLR7 genotype.
url http://europepmc.org/articles/PMC3192768?pdf=render
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