PLoS Pathogens (Oct 2019)

Effector memory differentiation increases detection of replication-competent HIV-l in resting CD4+ T cells from virally suppressed individuals.

  • Elizabeth R Wonderlich,
  • Krupa Subramanian,
  • Bryan Cox,
  • Ann Wiegand,
  • Carol Lackman-Smith,
  • Michael J Bale,
  • Mars Stone,
  • Rebecca Hoh,
  • Mary F Kearney,
  • Frank Maldarelli,
  • Steven G Deeks,
  • Michael P Busch,
  • Roger G Ptak,
  • Deanna A Kulpa

DOI
https://doi.org/10.1371/journal.ppat.1008074
Journal volume & issue
Vol. 15, no. 10
p. e1008074

Abstract

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Studies have demonstrated that intensive ART alone is not capable of eradicating HIV-1, as the virus rebounds within a few weeks upon treatment interruption. Viral rebound may be induced from several cellular subsets; however, the majority of proviral DNA has been found in antigen experienced resting CD4+ T cells. To achieve a cure for HIV-1, eradication strategies depend upon both understanding mechanisms that drive HIV-1 persistence as well as sensitive assays to measure the frequency of infected cells after therapeutic interventions. Assays such as the quantitative viral outgrowth assay (QVOA) measure HIV-1 persistence during ART by ex vivo activation of resting CD4+ T cells to induce latency reversal; however, recent studies have shown that only a fraction of replication-competent viruses are inducible by primary mitogen stimulation. Previous studies have shown a correlation between the acquisition of effector memory phenotype and HIV-1 latency reversal in quiescent CD4+ T cell subsets that harbor the reservoir. Here, we apply our mechanistic understanding that differentiation into effector memory CD4+ T cells more effectively promotes HIV-1 latency reversal to significantly improve proviral measurements in the QVOA, termed differentiation QVOA (dQVOA), which reveals a significantly higher frequency of the inducible HIV-1 replication-competent reservoir in resting CD4+ T cells.