Identification of Genetically Intact HIV-1 Proviruses in Specific CD4 + T Cells from Effectively Treated Participants

Hiener, Bonnie; Horsburgh, Bethany A.; Eden, John‐Sebastian; Barton, Kirston; Schlub, Timothy E.; Lee, Eun-Ok; Stockenström, Susanne von; Odevall, Lina; Milush, Jeffrey M.; Liegler, Teri; Sinclair, Elizabeth; Hoh, Rebecca; Boritz, Eli; Douek, Daniel C.; Fromentin, Rémi; Chomont, Nicolas; Deeks, Steven G.; Hecht, Frederick; Palmer, Sarah

doi:10.1016/j.celrep.2017.09.081

Cited by 323 publications

(558 citation statements)

References 40 publications

Supporting

Mentioning

484

Contrasting

Order By: Relevance

“…While it was originally believed by many that latently infected cells must be intrinsically long-lived, since cell division was expected to reactivate viral expression and lead to eventual cell death, a series of studies over the past few years have convincingly demonstrated that cells in the reservoir can proliferate while remaining latently infected (Reference 110,112). These studies have identified multiple latently infected cells -even in small samples -with virus integrated into identical sites [113][114][115] in the genome or with sequence-identical virus [116][117][118][119] -two findings that would be exceedingly unlikely to occur in two independent infection events and likely reflect division of infected cells.…”

Section: What Maintains the Latent Reservoir And How Can We Reducementioning

confidence: 99%

Insight into treatment ofHIVinfection from viral dynamics models

Hill

Rosenbloom

Nowak

et al. 2018

Immunological Reviews

View full text Add to dashboard Cite

SUMMARY The odds of living a long and healthy life with HIV infection have dramatically improved with the advent of combination antiretroviral therapy. Along with the early development and clinical trials of these drugs, and new field of research emerged called viral dynamics, which uses mathematical models to interpret and predict the time course of viral levels during infection and how they are altered by treatment. In this review, we summarize the contributions that virus dynamics models have made to understanding the pathophysiology of infection and to designing effective therapies. This includes studies of the multi-phasic decay of viral load when antiretroviral therapy is given, the evolution of drug resistance, the long-term persistence latently infected cells, and the rebound of viremia when drugs are stopped. We additionally discuss new work applying viral dynamics models to new classes of investigational treatment for HIV, including latency-reversing agents and immunotherapy.

show abstract

Section: What Maintains the Latent Reservoir And How Can We Reducementioning

confidence: 99%

Insight into treatment ofHIVinfection from viral dynamics models

Hill

Rosenbloom

Nowak

et al. 2018

Immunological Reviews

View full text Add to dashboard Cite

show abstract

“…The ability of HIV‐1 to primarily infect CD4+ memory T cells, but also infect naive cells is further supported by recent studies of viral reservoirs. Studies examining intact proviral genomes and quantitative viral outgrowth assays (QVOA) have found that HIV‐1 can persist in naive and memory CD4+ T cells in ART‐treated individuals regardless of whether individuals initiate therapy during acute or chronic infection. However, it is worth noting that the percentage of naive cells harboring replication‐competent proviral genomes is typically lower than that of memory T cells .…”

Section: Introductionmentioning

confidence: 99%

“…Studies examining intact proviral genomes and quantitative viral outgrowth assays (QVOA) have found that HIV‐1 can persist in naive and memory CD4+ T cells in ART‐treated individuals regardless of whether individuals initiate therapy during acute or chronic infection. However, it is worth noting that the percentage of naive cells harboring replication‐competent proviral genomes is typically lower than that of memory T cells . The fact that naive cells are less likely to be latently infected after a period of ART may be due to them being less susceptible to infection prior to therapy or due to them turning over more rapidly after the initiation of therapy.…”

Section: Introductionmentioning

confidence: 99%

The evolution of HIV-1 entry phenotypes as a guide to changing target cells

Joseph

Swanstrom

2018

Journal of Leukocyte Biology

View full text Add to dashboard Cite

Summary Sentence: The R5 T cell-tropic form of HIV-1 is the most abundant form and the evolutionary precursor to X4 T cell-tropic and macrophage-tropic variants. AbstractThrough a twist of fate the most common form of HIV-1, as defined by entry phenotype, was not appreciated until recently. The entry phenotype is closely linked to the target cell and thus to virus-host interactions and pathogenesis. The most abundant form of HIV-1 uses CCR5 as the coreceptor and requires a high density of CD4 for efficient entry, defining its target cell as the CD4+ memory T cell. This is the transmitted form of the virus, the form that is found in the blood, and the form that rebounds from the latent reservoir. When CD4+/CCR5+ T cells become limiting the virus evolves to use alternative target cells to support viral replication. In the CNS, the virus can evolve to use a cell that displays only a low density of CD4, while maintaining the use of CCR5 as the coreceptor. When this evolutionary variant evolves, it must be sustaining its replication in either macrophages or microglial cells, which display only a low density of CD4 relative to that on T cells. In the blood and lymphoid system, the major switch late in disease is from T cells expressing CD4 and CCR5 to T cells expressing CD4 and CXCR4, with a change in coreceptor specificity. Thus the virus responds in two different ways to different environments when its preferred target cell becomes limiting.

show abstract

“…Several recent studies have revealed important features of persistent HIV-1 that directly impact our understanding of the latent reservoir. Full viral genome sequencing studies have shown that over 93% of proviruses in resting CD4 + T cells in HIV + individuals on cART are defective (Ho et al 2013; Bruner et al 2016; Imamichi et al 2016; Hiener et al 2017; Lee et al 2017). These defective proviruses contain large internal deletions and/or hypermutation mediated by APOBEC3G, a host enzyme that deaminates dC to dU on the minus strand of HIV-1 cDNA during reverse transcription (resulting in a G to A hypermutation).…”

Section: A Historical Perspectivementioning

confidence: 99%

Targeting the Latent Reservoir for HIV-1

2018

View full text Add to dashboard Cite

Antiretroviral therapy can effectively block HIV-1 viral replication and prevent or reverse immunodeficiency in HIV-1-infected individuals. However, viral replication resumes within weeks of treatment interruption. The major barrier to cure is a small pool of resting memory CD4+ T cells that harbor latent HIV-1 proviruses. This latent reservoir is now the focus of an intense international research effort. We describe how the reservoir is established, challenges involved in eliminating it, and pharmacologic and immunologic strategies for targeting this reservoir. The development of a successful cure strategy will likely require understanding the mechanisms that maintain HIV-1 proviruses in a latent state and pathways that drive the proliferation of infected cells, which slows reservoir decay. In addition, cure will require the development of effective immunologic approaches to eliminating infected cells. There is renewed optimism about the prospect of a cure, and the interventions discussed here may pave the way.

show abstract

Identification of Genetically Intact HIV-1 Proviruses in Specific CD4 + T Cells from Effectively Treated Participants

Cited by 323 publications

References 40 publications

Insight into treatment ofHIVinfection from viral dynamics models

Insight into treatment ofHIVinfection from viral dynamics models

The evolution of HIV-1 entry phenotypes as a guide to changing target cells

Targeting the Latent Reservoir for HIV-1

Contact Info

Product

Resources

About