Mining for humoral correlates of HIV control and latent reservoir size.
While antiretroviral therapy (ART) has effectively revolutionized HIV care, the virus is never fully eliminated. Instead, immune dysfunction, driven by persistent non-specific immune activation, ensues and progressively leads to premature immunologic aging. Current biomarkers monitoring immunologic...
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Online Access: | https://doi.org/10.1371/journal.ppat.1008868 |
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doaj-3c9af2d7b9184bf88ad5e6cbfa43eb892021-07-13T04:30:51ZengPublic Library of Science (PLoS)PLoS Pathogens1553-73661553-73742020-10-011610e100886810.1371/journal.ppat.1008868Mining for humoral correlates of HIV control and latent reservoir size.Jishnu DasAnush DevadhasanCaitlyn LindeTom BrogeJessica SassicMax ManganoSean O'KeefeTodd SuscovichHendrik StreeckAlivelu IrrinkiChris PohlmeyerGundula Min-OoShu LinJoshua A WeinerThomas CihlarMargaret E AckermanBoris JulgSteven DeeksDouglas A LauffenburgerGalit AlterWhile antiretroviral therapy (ART) has effectively revolutionized HIV care, the virus is never fully eliminated. Instead, immune dysfunction, driven by persistent non-specific immune activation, ensues and progressively leads to premature immunologic aging. Current biomarkers monitoring immunologic changes encompass generic inflammatory biomarkers, that may also change with other infections or disease states, precluding the antigen-specific monitoring of HIV-infection associated changes in disease. Given our growing appreciation of the significant changes in qualitative and quantitative properties of disease-specific antibodies in HIV infection, we used a systems approach to explore humoral profiles associated with HIV control. We found that HIV-specific antibody profiles diverge by spontaneous control of HIV, treatment status, viral load and reservoir size. Specifically, HIV-specific antibody profiles representative of changes in viral load were largely quantitative, reflected by differential HIV-specific antibody levels and Fc-receptor binding. Conversely, HIV-specific antibody features that tracked with reservoir size exhibited a combination of quantitative and qualitative changes marked by more distinct subclass selection profiles and unique HIV-specific Fc-glycans. Our analyses suggest that HIV-specific antibody Fc-profiles provide antigen-specific resolution on both cell free and cell-associated viral loads, pointing to potentially novel biomarkers to monitor reservoir activity.https://doi.org/10.1371/journal.ppat.1008868 |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Jishnu Das Anush Devadhasan Caitlyn Linde Tom Broge Jessica Sassic Max Mangano Sean O'Keefe Todd Suscovich Hendrik Streeck Alivelu Irrinki Chris Pohlmeyer Gundula Min-Oo Shu Lin Joshua A Weiner Thomas Cihlar Margaret E Ackerman Boris Julg Steven Deeks Douglas A Lauffenburger Galit Alter |
spellingShingle |
Jishnu Das Anush Devadhasan Caitlyn Linde Tom Broge Jessica Sassic Max Mangano Sean O'Keefe Todd Suscovich Hendrik Streeck Alivelu Irrinki Chris Pohlmeyer Gundula Min-Oo Shu Lin Joshua A Weiner Thomas Cihlar Margaret E Ackerman Boris Julg Steven Deeks Douglas A Lauffenburger Galit Alter Mining for humoral correlates of HIV control and latent reservoir size. PLoS Pathogens |
author_facet |
Jishnu Das Anush Devadhasan Caitlyn Linde Tom Broge Jessica Sassic Max Mangano Sean O'Keefe Todd Suscovich Hendrik Streeck Alivelu Irrinki Chris Pohlmeyer Gundula Min-Oo Shu Lin Joshua A Weiner Thomas Cihlar Margaret E Ackerman Boris Julg Steven Deeks Douglas A Lauffenburger Galit Alter |
author_sort |
Jishnu Das |
title |
Mining for humoral correlates of HIV control and latent reservoir size. |
title_short |
Mining for humoral correlates of HIV control and latent reservoir size. |
title_full |
Mining for humoral correlates of HIV control and latent reservoir size. |
title_fullStr |
Mining for humoral correlates of HIV control and latent reservoir size. |
title_full_unstemmed |
Mining for humoral correlates of HIV control and latent reservoir size. |
title_sort |
mining for humoral correlates of hiv control and latent reservoir size. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS Pathogens |
issn |
1553-7366 1553-7374 |
publishDate |
2020-10-01 |
description |
While antiretroviral therapy (ART) has effectively revolutionized HIV care, the virus is never fully eliminated. Instead, immune dysfunction, driven by persistent non-specific immune activation, ensues and progressively leads to premature immunologic aging. Current biomarkers monitoring immunologic changes encompass generic inflammatory biomarkers, that may also change with other infections or disease states, precluding the antigen-specific monitoring of HIV-infection associated changes in disease. Given our growing appreciation of the significant changes in qualitative and quantitative properties of disease-specific antibodies in HIV infection, we used a systems approach to explore humoral profiles associated with HIV control. We found that HIV-specific antibody profiles diverge by spontaneous control of HIV, treatment status, viral load and reservoir size. Specifically, HIV-specific antibody profiles representative of changes in viral load were largely quantitative, reflected by differential HIV-specific antibody levels and Fc-receptor binding. Conversely, HIV-specific antibody features that tracked with reservoir size exhibited a combination of quantitative and qualitative changes marked by more distinct subclass selection profiles and unique HIV-specific Fc-glycans. Our analyses suggest that HIV-specific antibody Fc-profiles provide antigen-specific resolution on both cell free and cell-associated viral loads, pointing to potentially novel biomarkers to monitor reservoir activity. |
url |
https://doi.org/10.1371/journal.ppat.1008868 |
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