Intensification of Antiretroviral Therapy with a CCR5 Antagonist in Patients with Chronic HIV-1 Infection: Effect on T Cells Latently Infected

Gutiérrez, Carolina; Díaz, Laura; Vallejo, Alejandro; Hernández-Novoa, Beatriz; Abad, María Fernández; Madrid, Nadia; Dahl, Viktor; Rubio, Rafael; Moreno, Ana; Dronda, Fernando; Casado, José L.; Navas, Enrique; Pérez-Elías, María Jesús; Zamora, Javier; Palmer, Sarah; Muñóz, Eduardo; Muñoz‐Fernández, María Ángeles; Moreno, Santiago

doi:10.1371/journal.pone.0027864

Cited by 85 publications

(70 citation statements)

References 47 publications

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“…The decrease of D dimer levels which have been associated with lower cardiovascular risk in HIV-infected patients (4) could also be clinically relevant. However, these results contradict the increase in sCD14 levels observed after MVC intensification in a recent study (14). In fact, the higher levels found in that study were statistically significant after 24 to 48 weeks, but not at 12 weeks, on cART, and the previous study included a very different set of patients (under an MVC intensification strategy, on suppressive cART, and with much higher CD4 ϩ T-cell levels than patients in the present work).…”

Section: Discussioncontrasting

confidence: 99%

Effect of Maraviroc on HIV Disease Progression-Related Biomarkers

Romero-Sánchez

Machmach

González‐Serna

et al. 2012

Antimicrob Agents Chemother

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The potential effect of blocking the CCR5 receptor on HIV disease progression biomarkers is not well understood. We showed that an 8-day maraviroc (MVC) monotherapy clinical test (MCT) can be used in selecting patients to receive MVC-containing combined antiretroviral therapy (cART). Using this MCT model, we assessed the effect of MVC on several HIV disease progression biomarkers during the MCT (MVC-specific effect) and following short-term (12-week) cART. We compared 45 patients on MVC monotherapy with a control group of 25 patients on MVC-sparing cART. We found that MVC did not modify any biomarkers in patients that had no virological response after the MCT. MVC-specific effects in patients with virological responses included increased CD8 ؉ T-cell activation and senescence levels, preservation of an increase in soluble CD14 (sCD14), and a decrease in D dimer levels. After 12 weeks, MVC-containing cART increased CD8 ؉ T-cell counts and preserved CD4 ؉ T-cell senescence levels compared with MVC-sparing cART. Moreover, there was a decrease in sCD14 levels in patients that received MVCcontaining cART. In conclusion, effects compatible with CD8؉ T-cell redistribution in peripheral blood were observed after MVC therapy. However, MVC was associated with a favorable profile in HIV disease progression biomarkers only in patients with a virological response. These results support a potential clinical benefit of a therapy which includes MVC in HIV-infected patients.

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Section: Discussioncontrasting

confidence: 99%

Effect of Maraviroc on HIV Disease Progression-Related Biomarkers

Romero-Sánchez

Machmach

González‐Serna

et al. 2012

Antimicrob Agents Chemother

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“…[36][37][38][39] However, none of these studies was placebo-controlled, and subjects often improve their ART adherence when entering clinical trials, which may have explained the reduction in low-level viremia experienced by placebo-treated subjects in our own trial and in another recently reported intensification study. 40 The apparent reduction in T-cell activation during maraviroc intensification reported in the uncontrolled AIDS clinical trials group study (A5256) was also primarily driven by declines in CD38 expression, whereas HLA-DR expression actually increased significantly (which is largely consistent with our results), and neither of those changes were confirmed when retesting cryopreserved PBMCs from that trial.…”

Section: Discussionmentioning

confidence: 99%

The immunologic effects of maraviroc intensification in treated HIV-infected individuals with incomplete CD4+ T-cell recovery: a randomized trial

Hunt

Shulman

Hayes

et al. 2013

Blood

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127

123

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Key Points• Maraviroc intensification unexpectedly increases T-cell activation in peripheral blood and rectal mucosa during treated HIV infection.• Maraviroc appears to redistribute CD81 T cells from the gut to peripheral blood during treated HIV infection.The CCR5 inhibitor maraviroc has been hypothesized to decrease T-cell activation in HIVinfected individuals, but its independent immunologic effects have not been established in a placebo-controlled trial. We randomized 45 HIV-infected subjects with CD4 counts <350 cells per mm 3 and plasma HIV RNA levels <48 copies per mL on antiretroviral therapy (ART)to add maraviroc vs placebo to their regimen for 24 weeks followed by 12 weeks on ART alone. Compared with placebo-treated subjects, maraviroc-treated subjects unexpectedly experienced a greater median increase in % CD381HLA-DR1 peripheral blood CD81 T cells at week 24 (12.2% vs 20.7%, P 5 .014), and less of a decline in activated CD41 T cells (P < .001). The % CD381HLA-DR1 CD41 and CD81 T cells increased nearly twofold in rectal tissue (both P < .001), and plasma CC chemokine receptor type 5 (CCR5) ligand (macrophage-inflammatory protein 1b) levels increased 2.4-fold during maraviroc intensification (P < .001). During maraviroc intensification, plasma lipopolysaccharide declined, whereas sCD14 levels and neutrophils tended to increase in blood and rectal tissue. Although the mechanisms explaining these findings remain unclear, CCR5 ligandmediated activation of T cells, macrophages, and neutrophils via alternative chemokine receptors should be explored. These results may have relevance for trials of maraviroc for HIV preexposure prophylaxis and graft-versus-host disease. This trial was registered at www.clinicaltrials.gov as #NCT00735072. (Blood. 2013;121(23):4635-4646)

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“…We combined the data of two pilot open-label phase II clinical trials to evaluate the effect of maraviroc (ERRAD-VIH-01 (MRV): NCT00795444) 30 and raltegravir (ERRADVIH-02 (RAL): NCT00807443) 31 on the HIV latent reservoir. The studies were conducted at the Hospital Universitario Ram on y Cajal in Madrid, Spain, between 2008 and 2010.…”

Section: Study Design and Patientsmentioning

confidence: 99%

“…30,31 Briefly, PBMCs were isolated by Ficoll density gradient centrifugation (Lymphocytes Isolation Solution, Rafer, S.L., Zaragoza, Spain) from 300 mL of heparinised whole blood. Resting CD4 þ T-cells (CD3 þ /CD4 þ / HLADR À /CD25 À ) were then isolated and purified using magnetic beads according to the manufacturer's recommendations (Miltenyi Biotec GmbH., Bergisch Gladbach, Germany).…”

Section: Estimation Of the Hiv Latent Reservoirmentioning

confidence: 99%