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Cell-associated HIV-1 RNA predicts viral rebound and disease progression after discontinuation of temporary early ART
Alexander O. Pasternak, … , Jan M. Prins, Ben Berkhout
Alexander O. Pasternak, … , Jan M. Prins, Ben Berkhout
Published February 25, 2020
Citation Information: JCI Insight. 2020;5(6):e134196. https://doi.org/10.1172/jci.insight.134196.
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Research Article AIDS/HIV Virology

Cell-associated HIV-1 RNA predicts viral rebound and disease progression after discontinuation of temporary early ART

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Abstract

Plasma viral load (VL) and CD4+ T cell count are widely used as biomarkers of HIV type 1 (HIV-1) replication, pathogenesis, and response to antiretroviral therapy (ART). However, the clinical potential of cell-associated (CA) HIV-1 molecular markers is much less understood. Here, we measured CA HIV-1 RNA and DNA in HIV-infected individuals treated with temporary ART initiated during primary HIV-1 infection. We demonstrate substantial predictive value of CA RNA for (a) the virological and immunological response to early ART, (b) the magnitude and time to viral rebound after discontinuation of early ART, and (c) disease progression in the absence of treatment. Remarkably, when adjusted for CA RNA, plasma VL no longer appeared as an independent predictor of any clinical endpoint in this cohort. The potential of CA RNA as an HIV-1 clinical marker, in particular as a predictive biomarker of virological control after stopping ART, should be explored in the context of HIV-1 curative interventions.

Authors

Alexander O. Pasternak, Marlous L. Grijsen, Ferdinand W. Wit, Margreet Bakker, Suzanne Jurriaans, Jan M. Prins, Ben Berkhout

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Set point variables associated with the rates of disease progression (ti...

Set point variables associated with the rates of disease progression (time to CD4+ count < 350 cells/mm3 or restart ART) after virological set point (n = 56; Cox proportional hazards analysis)


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