Switching to boosted protease inhibitor plus a second antiretroviral drug (dual therapy) for treatment simplification: a multicenter analysis

BACKGROUND: To assess the role of drugs used in dual therapy (DT), as cART simplification, over the risk of treatment failure. MATERIALS AND METHODS: Patients starting DT regimen composed by a boosted protease inhibitor (PI/r): darunavir (DRV/r), lopinavir (LPVr) or atazanavir (ATV/r) plus a second...

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Autores principales: Zaccarelli, Mauro, Fabbiani, Massimiliano, Pinnetti, Carmela, Borghi, Vanni, Giannetti, Alberto, Sterrantino, Gaetana, Lorenzini, Patrizia, Latini, Alessandra, Loiacono, Laura, Colafigli, Manuela, Ammassari, Adriana, D'Ettorre, Gabriella, Plazzi, Maddalena, Di Giambenedetto, Simona, Antinori, Andrea
Formato: Online Artículo Texto
Lenguaje:English
Publicado: International AIDS Society 2014
Materias:
Poster Sessions – Abstract P270
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4225349/
https://www.ncbi.nlm.nih.gov/pubmed/25397546
http://dx.doi.org/10.7448/IAS.17.4.19802
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author Zaccarelli, Mauro
Fabbiani, Massimiliano
Pinnetti, Carmela
Borghi, Vanni
Giannetti, Alberto
Sterrantino, Gaetana
Lorenzini, Patrizia
Latini, Alessandra
Loiacono, Laura
Colafigli, Manuela
Ammassari, Adriana
D'Ettorre, Gabriella
Plazzi, Maddalena
Di Giambenedetto, Simona
Antinori, Andrea
author_facet Zaccarelli, Mauro
Fabbiani, Massimiliano
Pinnetti, Carmela
Borghi, Vanni
Giannetti, Alberto
Sterrantino, Gaetana
Lorenzini, Patrizia
Latini, Alessandra
Loiacono, Laura
Colafigli, Manuela
Ammassari, Adriana
D'Ettorre, Gabriella
Plazzi, Maddalena
Di Giambenedetto, Simona
Antinori, Andrea
author_sort Zaccarelli, Mauro
collection PubMed
description BACKGROUND: To assess the role of drugs used in dual therapy (DT), as cART simplification, over the risk of treatment failure. MATERIALS AND METHODS: Patients starting DT regimen composed by a boosted protease inhibitor (PI/r): darunavir (DRV/r), lopinavir (LPVr) or atazanavir (ATV/r) plus a second drug: raltegravir (RAL), maraviroc (MRV) etravirine (ETR), lamivudine (3TC) or tenofovir (TDF), this one generally used in HBV co-infected patients, were included. The effect of each drug as well as other clinical and virological cofactors over treatment failure was assessed using survival analysis. RESULTS: Overall, 480 patients from six reference Italian centres were included: all switched to DT with HIV-RNA <500 cp/µL, 376 of them at <50 cp/µL. Patients who switched at <50 cp/µL showed a significant lower risk of treatment failure (13.3% versus 23.3% at 1 year and 28.0% versus 44.6% at 3 years, p=0.005), thus the analysis was focused on this subgroup. Among the patients who switched at <50 cp/µL, the proportion of drug used in DT was: DRV/r 63.0%, RAL 53.7%, ETR 19.4%, ATV/r 18.4%, MRV 17.3%, LPV/r 12.8%, TDF 6.4% and 3TC 5.9%; DRV/r-RAL was the most widely used combination: 32.5%. Treatment failure was observed in 78 patients, of whom 38 virological and 35 for toxicity/intolerance, one patient died during follow-up and four patients interrupted for personal decision with undetectable HIV-RNA. At Cox Model, adjusted by gender, age, non-Italian origin, AIDS diagnosis, time on cART, number of regimens, CD4 nadir, baseline CD4, all the drugs had a positive effect on probability of failure (Figure), however the effect was significant for DRV/r (HR:0.21, 95% CI 0.07–0.59, p=0.03), ATV/r (0.30, 0.09–0.97, p=0.044) and RAL (0.37, 0.15–0.93, p=0.034); higher CD4 count at baseline was also associated with lower risk of failure while number of previous regimens with a higher risk. Moreover, ATV/r was found significant associated with significant higher risk of failure by toxicity (as well as LPV/r) but lower risk of virological failure, while both 3TC and RAL with significant lower risk of toxicity. CONCLUSIONS: Our analysis suggest that using PI/r-based DL is highly effective if switching from HIV-RNA <50 cp/µL; DL should be used with caution in patients with low CD4 count and longer history of treatment; DRV/r is the best compromise among PI/r, ATV/r is effective but is associate with frequent interruption by toxicity; RAL showed high tolerability so that its use is related to the lowest risk of failure as second drug.
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spelling pubmed-42253492014-11-13 Switching to boosted protease inhibitor plus a second antiretroviral drug (dual therapy) for treatment simplification: a multicenter analysis Zaccarelli, Mauro Fabbiani, Massimiliano Pinnetti, Carmela Borghi, Vanni Giannetti, Alberto Sterrantino, Gaetana Lorenzini, Patrizia Latini, Alessandra Loiacono, Laura Colafigli, Manuela Ammassari, Adriana D'Ettorre, Gabriella Plazzi, Maddalena Di Giambenedetto, Simona Antinori, Andrea J Int AIDS Soc Poster Sessions – Abstract P270 BACKGROUND: To assess the role of drugs used in dual therapy (DT), as cART simplification, over the risk of treatment failure. MATERIALS AND METHODS: Patients starting DT regimen composed by a boosted protease inhibitor (PI/r): darunavir (DRV/r), lopinavir (LPVr) or atazanavir (ATV/r) plus a second drug: raltegravir (RAL), maraviroc (MRV) etravirine (ETR), lamivudine (3TC) or tenofovir (TDF), this one generally used in HBV co-infected patients, were included. The effect of each drug as well as other clinical and virological cofactors over treatment failure was assessed using survival analysis. RESULTS: Overall, 480 patients from six reference Italian centres were included: all switched to DT with HIV-RNA <500 cp/µL, 376 of them at <50 cp/µL. Patients who switched at <50 cp/µL showed a significant lower risk of treatment failure (13.3% versus 23.3% at 1 year and 28.0% versus 44.6% at 3 years, p=0.005), thus the analysis was focused on this subgroup. Among the patients who switched at <50 cp/µL, the proportion of drug used in DT was: DRV/r 63.0%, RAL 53.7%, ETR 19.4%, ATV/r 18.4%, MRV 17.3%, LPV/r 12.8%, TDF 6.4% and 3TC 5.9%; DRV/r-RAL was the most widely used combination: 32.5%. Treatment failure was observed in 78 patients, of whom 38 virological and 35 for toxicity/intolerance, one patient died during follow-up and four patients interrupted for personal decision with undetectable HIV-RNA. At Cox Model, adjusted by gender, age, non-Italian origin, AIDS diagnosis, time on cART, number of regimens, CD4 nadir, baseline CD4, all the drugs had a positive effect on probability of failure (Figure), however the effect was significant for DRV/r (HR:0.21, 95% CI 0.07–0.59, p=0.03), ATV/r (0.30, 0.09–0.97, p=0.044) and RAL (0.37, 0.15–0.93, p=0.034); higher CD4 count at baseline was also associated with lower risk of failure while number of previous regimens with a higher risk. Moreover, ATV/r was found significant associated with significant higher risk of failure by toxicity (as well as LPV/r) but lower risk of virological failure, while both 3TC and RAL with significant lower risk of toxicity. CONCLUSIONS: Our analysis suggest that using PI/r-based DL is highly effective if switching from HIV-RNA <50 cp/µL; DL should be used with caution in patients with low CD4 count and longer history of treatment; DRV/r is the best compromise among PI/r, ATV/r is effective but is associate with frequent interruption by toxicity; RAL showed high tolerability so that its use is related to the lowest risk of failure as second drug. International AIDS Society 2014-11-02 /pmc/articles/PMC4225349/ /pubmed/25397546 http://dx.doi.org/10.7448/IAS.17.4.19802 Text en © 2014 Pironti A et al; licensee International AIDS Society http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Poster Sessions – Abstract P270
Zaccarelli, Mauro
Fabbiani, Massimiliano
Pinnetti, Carmela
Borghi, Vanni
Giannetti, Alberto
Sterrantino, Gaetana
Lorenzini, Patrizia
Latini, Alessandra
Loiacono, Laura
Colafigli, Manuela
Ammassari, Adriana
D'Ettorre, Gabriella
Plazzi, Maddalena
Di Giambenedetto, Simona
Antinori, Andrea
Switching to boosted protease inhibitor plus a second antiretroviral drug (dual therapy) for treatment simplification: a multicenter analysis
title Switching to boosted protease inhibitor plus a second antiretroviral drug (dual therapy) for treatment simplification: a multicenter analysis
title_full Switching to boosted protease inhibitor plus a second antiretroviral drug (dual therapy) for treatment simplification: a multicenter analysis
title_fullStr Switching to boosted protease inhibitor plus a second antiretroviral drug (dual therapy) for treatment simplification: a multicenter analysis
title_full_unstemmed Switching to boosted protease inhibitor plus a second antiretroviral drug (dual therapy) for treatment simplification: a multicenter analysis
title_short Switching to boosted protease inhibitor plus a second antiretroviral drug (dual therapy) for treatment simplification: a multicenter analysis
title_sort switching to boosted protease inhibitor plus a second antiretroviral drug (dual therapy) for treatment simplification: a multicenter analysis
topic Poster Sessions – Abstract P270
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4225349/
https://www.ncbi.nlm.nih.gov/pubmed/25397546
http://dx.doi.org/10.7448/IAS.17.4.19802
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