VS411 Reduced Immune Activation and HIV-1 RNA Levels in 28 Days: Randomized Proof-of-Concept Study for AntiViral-HyperActivation Limiting Therapeutics

Friedman, Lori S.; Forni, Davide De; Katabira, Elly; Baev, Denis; Maserati, Renato; Calarota, Sandra A.; Cahn, Pedro; Testori, Marco; Rakhmanova, Aza; Stevens, Michael R.

doi:10.1371/journal.pone.0047485

Cited by 3 publications

(3 citation statements)

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“…Suboptimal responders pose several clinical questions, including questions about the clinical risk associated with persistent immunodeficiency and about possible interventions to optimise clinical and immunological benefits of HAART [12,30]. From a clinical point of view, it is reasonable to hypothesise that adjuvant therapy with anti-immune activation agents [31,32] may improve T-cell proliferation potential among suboptimal responders. Our work presents an interface between clinical care and basic science research.…”

Section: Discussionmentioning

confidence: 99%

Impaired T-cell proliferation among HAART-treated adults with suboptimal CD4 recovery in an African cohort

et al. 2013

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BackgroundMost HIV-infected subjects exhibit a progressive rise in CD4 T-cell counts after initiation of highly active antiretroviral therapy (HAART). However, a subset of individuals exhibit very poor CD4 T-cell recovery despite effective control of HIV-RNA viraemia. We evaluated CD4 T-cell proliferation among suboptimal responders and its correlation with CD4 T-cell activation.MethodsThe magnitude of CD4 increase (difference between absolute CD4 counts at baseline and absolute CD4 counts at 4 years of ART) was grouped into 4 quartiles for the 211 patients with sustained HIV-RNA viral suppression. Cases of ‘Suboptimal immune responders’ included patients within the lowest quartile [Median CD4 increase 165 (Range −43-298) cells/μl; n=52] and a comparison group of ‘Optimal immune responders’ was defined as patients within the highest quartile of CD4 increase [Median CD4 increase 528 (Range 417–878) cells/μl; n=52]. Frozen PBMC were thawed and analysed from a convenient sample of 39 suboptimal responders and 48 optimal responders after 4 years of suppressive antiretroviral therapy. T-cell activation was measured by proportions of T-cells expressing surface marker CD38 and HLADR (CD4+CD38+HLA-DR+ and CD8+CD38+HLA-DR+ cells). T-cell proliferation was determined by the extent of carboxyfluorescein diacetate succinimidyl ester (CFSE) dye dilution on culture day 5 of PBMCs in the presence of antigen (SEB, PPD, CMVpp65, GagA and GagD). Samples were analyzed on a FACS Calibur flow cytometer and flow data was analyzed using FlowJo and GraphPad.ResultsOverall, CD4 T-cell proliferation on stimulation with SEB, PPD, CMVpp65, Gag A and Gag D.antigens, was lower among suboptimal than optimal responders; this was significant for SEB (CD4+ p=0.003; CD8+ p=0.048) and PPD antigens (CD8+ p=0.038). Among suboptimal responders, T-cell proliferation decreased with increasing immune activation (Negative correlation; slope = −0.13±−0.11) but not among optimal responders.ConclusionT-cell immune activation and exhaustion were associated with poor proliferation among suboptimal responders to HAART despite sustained viral suppression. We recommend studies to further understand the mechanisms leading to impaired T-cell function among suboptimal responders as well as the potential role of immune modulation in optimizing CD4 count and functional recovery after HAART.

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Section: Discussionmentioning

confidence: 99%

Impaired T-cell proliferation among HAART-treated adults with suboptimal CD4 recovery in an African cohort

et al. 2013

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“…Despite its promises, hydroxyurea treatment was shown to provoke complications, such as blunted CD4+ T cell recovery and severe toxicity, in HIV infected patients (Bloch et al, 2006;Zala et al, 2002). Recent studies suggest that these undesirable effects were due to a too high dose of the drug, and that both the antiviral and the cytostatic activities of hydroxyurea may contribute to control HIV when used at lower concentrations (Lori et al, 2012).…”

Section: Innovative Approaches To Eliminate Hiv Reservoirsmentioning

confidence: 99%

HIV cure research: Advances and prospects

2014

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Thirty years after the identification of HIV, a cure for HIV infection is still to be achieved. Advances of combined antiretroviral therapy (cART) in recent years have transformed HIV infection into a chronic disease when treatment is available. However, in spite of the favorable outcomes provided by the newer therapies, cART is not curative and patients are at risk of developing HIV-associated disorders. Moreover, universal access to antiretroviral treatment is restricted by financial obstacles. This review discusses the most recent strategies that have been developed in the search for an HIV cure and to improve life quality of people living with HIV.

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“…This effect may hamper viral reservoir maintenance/expansion in T CM and T TM cells that mainly relies on antigen-driven and homeostatic proliferation respectively [ 12 ]. Despite these promising results, combinations of hydroxyurea and antiretroviral drugs displayed in some instances high pancreatic and hepatic toxicity [ 20 , 21 ] and consequently hydroxyurea is not recommended for routine treatment of HIV infection, although there is still ongoing research on this topic [ 22 ].…”

Section: Reviewmentioning

confidence: 99%

A cure for AIDS: a matter of timing?

Shytaj

Savarino

2013

Retrovirology

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Despite the huge clinical success of antiretroviral therapy, several factors such as side effects, requirement of life-long adherence, high cost, incomplete access to therapies and development of drug resistance make the quest for an ultimate cure of HIV/AIDS a worldwide priority of biomedical research. In this respect, several sterilizing or functional cures have been reported in the last years in both non-human primates and humans. This review provides a summary of the main results achieved so far, outlining their strengths as well as their limitations. A synthetic interpretation of these results could be pivotal in order to develop an effective and widely available cure.

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VS411 Reduced Immune Activation and HIV-1 RNA Levels in 28 Days: Randomized Proof-of-Concept Study for AntiViral-HyperActivation Limiting Therapeutics

Cited by 3 publications

References 45 publications

Impaired T-cell proliferation among HAART-treated adults with suboptimal CD4 recovery in an African cohort

Impaired T-cell proliferation among HAART-treated adults with suboptimal CD4 recovery in an African cohort

HIV cure research: Advances and prospects

A cure for AIDS: a matter of timing?

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