4.7 Article

Longitudinal Genetic Characterization Reveals That Cell Proliferation Maintains a Persistent HIV Type 1 DNA Pool During Effective HIV Therapy

Journal

JOURNAL OF INFECTIOUS DISEASES
Volume 212, Issue 4, Pages 596-607

Publisher

OXFORD UNIV PRESS INC
DOI: 10.1093/infdis/jiv092

Keywords

HIV-1 persistence; HIV-1 reservoir; memory T cells

Funding

  1. Foundation for AIDS Research (amfAR Research Consortium on HIV Eradication Collaborative research grant) [108074-50-RGRL]
  2. Delaney AIDS Research Enterprise [U19 AI096109]
  3. Australian National Health and Medical Research Council [AAP1061681]
  4. Erik and Edith Fernstrom Foundation for Medical Research
  5. Karolinska Institutet

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Background. The stability of the human immunodeficiency virus type 1 (HIV-1) reservoir and the contribution of cellular proliferation to the maintenance of the reservoir during treatment are uncertain. Therefore, we conducted a longitudinal analysis of HIV-1 in T-cell subsets in different tissue compartments from subjects receiving effective antiretroviral therapy (ART). Methods. Using single-proviral sequencing, we isolated intracellular HIV-1 genomes derived from defined subsets of CD4+ T cells from peripheral blood, gut-associated lymphoid tissue and lymph node tissue specimens from 8 subjects with virologic suppression during long-term ART at 2 time points (time points 1 and 2) separated by 7-9 months. Results. DNA integrant frequencies were stable over time (<4-fold difference) and highest in memory T cells. Phylogenetic analyses showed that subjects treated during chronic infection contained viral populations with up to 73% identical sequence expansions, only 3 of which were observed in specimens obtained before therapy. At time points 1 and 2, such clonally expanded populations were found predominantly in effector memory T cells from peripheral blood and lymph node tissue specimens. Conclusions. Memory T cells maintained a relatively constant HIV-1 DNA integrant pool that was genetically stable during long-term effective ART. These integrants appear to be maintained by cellular proliferation and longevity of infected cells, rather than by ongoing viral replication.

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