Author:
Martin Genevieve E,Pace Matthew,Thornhill John P,Phetsouphanh Chansavath,Meyerowitz Jodi,Gossez Morgane,Hopkins Emily,Brown Helen,Robinson Nicola,Olejniczak Natalia,Ramjee Gita,Kaleebu Pontiano,Porter Kholoud,Willberg Christian,Klenerman Paul,Nwokolo Nneka,Fox Julie,Fidler Sarah,Frater John
Abstract
AbstractThe Fc receptor CD32 has been proposed as a marker for CD4 T cells latently infected with HIV. We demonstrate that enrichment for HIV DNA in CD32+ CD4 T cells can be found early in infection in both tissue and blood. However, we find no evidence for a correlation between CD32 expression on CD4 T cells and either HIV DNA levels or time to rebound viraemia following treatment interruption. CD32+ CD4 T cells have a more differentiated memory phenotype, and high levels of expression of immune checkpoint receptors PD-1, Tim-3 and TIGIT as well as the activation marker, HLA DR. There was no difference in the phenotype or frequency of CD32 expressing cells prior to or after the initiation of antiretroviral therapy, or compared with healthy controls, suggesting that preferential infection or survival, rather than up-regulation, may be responsible for the observed enrichment of proviral HIV DNA in CD32+ CD4 T cells.
Publisher
Cold Spring Harbor Laboratory
Cited by
2 articles.
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