Role of Transmitted Gag CTL Polymorphisms in Defining Replicative Capacity and Early HIV-1 Pathogenesis

Initial studies of 88 transmission pairs in the Zambia Emory HIV Research Project cohort demonstrated that the number of transmitted HLA-B associated polymorphisms in Gag, but not Nef, was negatively correlated to set point viral load (VL) in the newly infected partners. These results suggested that...

Descripción completa

Detalles Bibliográficos
Autores principales: Prince, Jessica L., Claiborne, Daniel T., Carlson, Jonathan M., Schaefer, Malinda, Yu, Tianwei, Lahki, Shabir, Prentice, Heather A., Yue, Ling, Vishwanathan, Sundaram A., Kilembe, William, Goepfert, Paul, Price, Matthew A., Gilmour, Jill, Mulenga, Joseph, Farmer, Paul, Derdeyn, Cynthia A., Tang, Jiaming, Heckerman, David, Kaslow, Richard A., Allen, Susan A., Hunter, Eric
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3510241/
https://www.ncbi.nlm.nih.gov/pubmed/23209412
http://dx.doi.org/10.1371/journal.ppat.1003041
_version_ 1782251441082073088
author Prince, Jessica L.
Claiborne, Daniel T.
Carlson, Jonathan M.
Schaefer, Malinda
Yu, Tianwei
Lahki, Shabir
Prentice, Heather A.
Yue, Ling
Vishwanathan, Sundaram A.
Kilembe, William
Goepfert, Paul
Price, Matthew A.
Gilmour, Jill
Mulenga, Joseph
Farmer, Paul
Derdeyn, Cynthia A.
Tang, Jiaming
Heckerman, David
Kaslow, Richard A.
Allen, Susan A.
Hunter, Eric
author_facet Prince, Jessica L.
Claiborne, Daniel T.
Carlson, Jonathan M.
Schaefer, Malinda
Yu, Tianwei
Lahki, Shabir
Prentice, Heather A.
Yue, Ling
Vishwanathan, Sundaram A.
Kilembe, William
Goepfert, Paul
Price, Matthew A.
Gilmour, Jill
Mulenga, Joseph
Farmer, Paul
Derdeyn, Cynthia A.
Tang, Jiaming
Heckerman, David
Kaslow, Richard A.
Allen, Susan A.
Hunter, Eric
author_sort Prince, Jessica L.
collection PubMed
description Initial studies of 88 transmission pairs in the Zambia Emory HIV Research Project cohort demonstrated that the number of transmitted HLA-B associated polymorphisms in Gag, but not Nef, was negatively correlated to set point viral load (VL) in the newly infected partners. These results suggested that accumulation of CTL escape mutations in Gag might attenuate viral replication and provide a clinical benefit during early stages of infection. Using a novel approach, we have cloned gag sequences isolated from the earliest seroconversion plasma sample from the acutely infected recipient of 149 epidemiologically linked Zambian transmission pairs into a primary isolate, subtype C proviral vector, MJ4. We determined the replicative capacity (RC) of these Gag-MJ4 chimeras by infecting the GXR25 cell line and quantifying virion production in supernatants via a radiolabeled reverse transcriptase assay. We observed a statistically significant positive correlation between RC conferred by the transmitted Gag sequence and set point VL in newly infected individuals (p = 0.02). Furthermore, the RC of Gag-MJ4 chimeras also correlated with the VL of chronically infected donors near the estimated date of infection (p = 0.01), demonstrating that virus replication contributes to VL in both acute and chronic infection. These studies also allowed for the elucidation of novel sites in Gag associated with changes in RC, where rare mutations had the greatest effect on fitness. Although we observed both advantageous and deleterious rare mutations, the latter could point to vulnerable targets in the HIV-1 genome. Importantly, RC correlated significantly (p = 0.029) with the rate of CD4+ T cell decline over the first 3 years of infection in a manner that is partially independent of VL, suggesting that the replication capacity of HIV-1 during the earliest stages of infection is a determinant of pathogenesis beyond what might be expected based on set point VL alone.
format Online
Article
Text
id pubmed-3510241
institution National Center for Biotechnology Information
language English
publishDate 2012
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-35102412012-12-03 Role of Transmitted Gag CTL Polymorphisms in Defining Replicative Capacity and Early HIV-1 Pathogenesis Prince, Jessica L. Claiborne, Daniel T. Carlson, Jonathan M. Schaefer, Malinda Yu, Tianwei Lahki, Shabir Prentice, Heather A. Yue, Ling Vishwanathan, Sundaram A. Kilembe, William Goepfert, Paul Price, Matthew A. Gilmour, Jill Mulenga, Joseph Farmer, Paul Derdeyn, Cynthia A. Tang, Jiaming Heckerman, David Kaslow, Richard A. Allen, Susan A. Hunter, Eric PLoS Pathog Research Article Initial studies of 88 transmission pairs in the Zambia Emory HIV Research Project cohort demonstrated that the number of transmitted HLA-B associated polymorphisms in Gag, but not Nef, was negatively correlated to set point viral load (VL) in the newly infected partners. These results suggested that accumulation of CTL escape mutations in Gag might attenuate viral replication and provide a clinical benefit during early stages of infection. Using a novel approach, we have cloned gag sequences isolated from the earliest seroconversion plasma sample from the acutely infected recipient of 149 epidemiologically linked Zambian transmission pairs into a primary isolate, subtype C proviral vector, MJ4. We determined the replicative capacity (RC) of these Gag-MJ4 chimeras by infecting the GXR25 cell line and quantifying virion production in supernatants via a radiolabeled reverse transcriptase assay. We observed a statistically significant positive correlation between RC conferred by the transmitted Gag sequence and set point VL in newly infected individuals (p = 0.02). Furthermore, the RC of Gag-MJ4 chimeras also correlated with the VL of chronically infected donors near the estimated date of infection (p = 0.01), demonstrating that virus replication contributes to VL in both acute and chronic infection. These studies also allowed for the elucidation of novel sites in Gag associated with changes in RC, where rare mutations had the greatest effect on fitness. Although we observed both advantageous and deleterious rare mutations, the latter could point to vulnerable targets in the HIV-1 genome. Importantly, RC correlated significantly (p = 0.029) with the rate of CD4+ T cell decline over the first 3 years of infection in a manner that is partially independent of VL, suggesting that the replication capacity of HIV-1 during the earliest stages of infection is a determinant of pathogenesis beyond what might be expected based on set point VL alone. Public Library of Science 2012-11-29 /pmc/articles/PMC3510241/ /pubmed/23209412 http://dx.doi.org/10.1371/journal.ppat.1003041 Text en © 2012 Prince et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Prince, Jessica L.
Claiborne, Daniel T.
Carlson, Jonathan M.
Schaefer, Malinda
Yu, Tianwei
Lahki, Shabir
Prentice, Heather A.
Yue, Ling
Vishwanathan, Sundaram A.
Kilembe, William
Goepfert, Paul
Price, Matthew A.
Gilmour, Jill
Mulenga, Joseph
Farmer, Paul
Derdeyn, Cynthia A.
Tang, Jiaming
Heckerman, David
Kaslow, Richard A.
Allen, Susan A.
Hunter, Eric
Role of Transmitted Gag CTL Polymorphisms in Defining Replicative Capacity and Early HIV-1 Pathogenesis
title Role of Transmitted Gag CTL Polymorphisms in Defining Replicative Capacity and Early HIV-1 Pathogenesis
title_full Role of Transmitted Gag CTL Polymorphisms in Defining Replicative Capacity and Early HIV-1 Pathogenesis
title_fullStr Role of Transmitted Gag CTL Polymorphisms in Defining Replicative Capacity and Early HIV-1 Pathogenesis
title_full_unstemmed Role of Transmitted Gag CTL Polymorphisms in Defining Replicative Capacity and Early HIV-1 Pathogenesis
title_short Role of Transmitted Gag CTL Polymorphisms in Defining Replicative Capacity and Early HIV-1 Pathogenesis
title_sort role of transmitted gag ctl polymorphisms in defining replicative capacity and early hiv-1 pathogenesis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3510241/
https://www.ncbi.nlm.nih.gov/pubmed/23209412
http://dx.doi.org/10.1371/journal.ppat.1003041
work_keys_str_mv AT princejessical roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT claibornedanielt roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT carlsonjonathanm roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT schaefermalinda roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT yutianwei roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT lahkishabir roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT prenticeheathera roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT yueling roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT vishwanathansundarama roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT kilembewilliam roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT goepfertpaul roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT pricematthewa roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT gilmourjill roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT mulengajoseph roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT farmerpaul roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT derdeyncynthiaa roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT tangjiaming roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT heckermandavid roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT kaslowricharda roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT allensusana roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis
AT huntereric roleoftransmittedgagctlpolymorphismsindefiningreplicativecapacityandearlyhiv1pathogenesis

Ejemplares similares