Efficacy and tolerability of lamivudine plus dolutegravir compared with lamivudine plus boosted PIs in HIV-1 positive individuals with virologic suppression: a retrospective study from the clinical practice.

Adult Anti-HIV Agents / administration & dosage Antiretroviral Therapy, Highly Active / adverse effects Atazanavir Sulfate / therapeutic use Cohort Studies Darunavir / therapeutic use Drug Therapy, Combination Female HIV Infections / drug therapy HIV Seropositivity / drug therapy HIV-1 / drug effects Heterocyclic Compounds, 3-Ring / administration & dosage Humans Lamivudine / administration & dosage Male Middle Aged Oxazines Piperazines Pyridones Retrospective Studies Ritonavir / therapeutic use Tenofovir / therapeutic use Treatment Outcome Viral Load / drug effects
Antiretroviral therapy Atazanavir/ritonavir Darunavir/ritonavir Dolutegravir Dual therapy HIV Lamivudine Maintenance therapy

Journal

BMC infectious diseases
ISSN: 1471-2334
Titre abrégé: BMC Infect Dis
Pays: England
ID NLM: 100968551

Informations de publication

Date de publication:
17 Jan 2019
Historique:
received: 13 01 2018
accepted: 28 12 2018
entrez: 19 1 2019
pubmed: 19 1 2019
medline: 7 3 2019
Statut: epublish

Résumé

Direct comparisons between lamivudine plus bPIs and lamivudine plus dolutegravir as maintenance strategies in virologically-suppressed HIV positive patients are lacking. Time to treatment discontinuation (TD) and virological failure (VF) were compared in a cohort of HIV+ patients on a virologically-effective ART starting lamivudine with either darunavir/r, atazanavir/r or dolutegravir. Changes in laboratory parameters were also evaluated. Four-hundred-ninety-four patients were analyzed (170 switching to darunavir/r, 141 to atazanavir/r, 183 to dolutegravir): median age was 49 years, with 8 years since ART start. Groups differed for age, HIV-risk factor, time since HIV-diagnosis and on ART, previous therapy and reasons for switching. Estimated proportions free from TD at week 48 and 96 were 79.8 and 48.3% of patients with darunavir/r, 87.0 and 70.9% with atazanavir/r, and 88.2 and 82.6% with dolutegravir, respectively (p < 0.001). Calendar years, HIV-risk factor, higher baseline cholesterol and an InSTI-based previous regimen predicted TD, whereas lamivudine+dolutegravir therapy and previous tenofovir use were protective. VF was the cause of TD in 6/123 cases with darunavir/r, 4/97 with atazanavir/r and 3/21 with dolutegravir. Other main reasons for TD were: toxicity (43.1% with darunavir/r, 39.2% with atazanavir/r, 52.4% with dolutegravir), further simplification (36.6% with darunavir/r, 30.9% with atazanavir/r, 14.3% with dolutegravir). Incidence of VF did not differ among study groups (p = 0.747). No factor could predict VF. Lipid profile improved in the dolutegravir group, whereas renal function improved in the bPIs groups. In real practice, a switch to lamivudine+dolutegravir showed similar efficacy but longer durability than a switch to lamivudine+bPIs.

Sections du résumé

BACKGROUND BACKGROUND
Direct comparisons between lamivudine plus bPIs and lamivudine plus dolutegravir as maintenance strategies in virologically-suppressed HIV positive patients are lacking.
METHODS METHODS
Time to treatment discontinuation (TD) and virological failure (VF) were compared in a cohort of HIV+ patients on a virologically-effective ART starting lamivudine with either darunavir/r, atazanavir/r or dolutegravir. Changes in laboratory parameters were also evaluated.
RESULTS RESULTS
Four-hundred-ninety-four patients were analyzed (170 switching to darunavir/r, 141 to atazanavir/r, 183 to dolutegravir): median age was 49 years, with 8 years since ART start. Groups differed for age, HIV-risk factor, time since HIV-diagnosis and on ART, previous therapy and reasons for switching. Estimated proportions free from TD at week 48 and 96 were 79.8 and 48.3% of patients with darunavir/r, 87.0 and 70.9% with atazanavir/r, and 88.2 and 82.6% with dolutegravir, respectively (p < 0.001). Calendar years, HIV-risk factor, higher baseline cholesterol and an InSTI-based previous regimen predicted TD, whereas lamivudine+dolutegravir therapy and previous tenofovir use were protective. VF was the cause of TD in 6/123 cases with darunavir/r, 4/97 with atazanavir/r and 3/21 with dolutegravir. Other main reasons for TD were: toxicity (43.1% with darunavir/r, 39.2% with atazanavir/r, 52.4% with dolutegravir), further simplification (36.6% with darunavir/r, 30.9% with atazanavir/r, 14.3% with dolutegravir). Incidence of VF did not differ among study groups (p = 0.747). No factor could predict VF. Lipid profile improved in the dolutegravir group, whereas renal function improved in the bPIs groups.
CONCLUSIONS CONCLUSIONS
In real practice, a switch to lamivudine+dolutegravir showed similar efficacy but longer durability than a switch to lamivudine+bPIs.

Identifiants

DOI: 10.1186/s12879-018-3666-8 PMID: 30654739 PMC: PMC6335713
pubmed: 30654739
doi: 10.1186/s12879-018-3666-8
pii: 10.1186/s12879-018-3666-8
pmc: PMC6335713
doi:

Substances chimiques

Anti-HIV Agents 0
Heterocyclic Compounds, 3-Ring 0
Oxazines 0
Piperazines 0
Pyridones 0
Lamivudine 2T8Q726O95
Atazanavir Sulfate 4MT4VIE29P
Tenofovir 99YXE507IL
dolutegravir DKO1W9H7M1
Ritonavir O3J8G9O825
Darunavir YO603Y8113

Types de publication

Comparative Study Journal Article

Langues

eng

Sous-ensembles de citation

IM

Pagination

59

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Auteurs

Alberto Borghetti (A)

Institute of Clinical Infectious Diseases, Catholic University of Sacred Heart, Policlinico Gemelli, Rome, Italy.

Francesca Lombardi (F)

Institute of Clinical Infectious Diseases, Catholic University of Sacred Heart, Policlinico Gemelli, Rome, Italy.

Roberta Gagliardini (R)

Infectious Diseases Unit, Siena University Hospital, Viale Mario Bracci, 53100, Siena, Italy.

Gianmaria Baldin (G)

Institute of Clinical Infectious Diseases, Catholic University of Sacred Heart, Policlinico Gemelli, Rome, Italy.

Arturo Ciccullo (A)

Institute of Clinical Infectious Diseases, Catholic University of Sacred Heart, Policlinico Gemelli, Rome, Italy.

Davide Moschese (D)

Institute of Clinical Infectious Diseases, Catholic University of Sacred Heart, Policlinico Gemelli, Rome, Italy.

Arianna Emiliozzi (A)

Institute of Clinical Infectious Diseases, Catholic University of Sacred Heart, Policlinico Gemelli, Rome, Italy.

Simone Belmonti (S)

Institute of Clinical Infectious Diseases, Catholic University of Sacred Heart, Policlinico Gemelli, Rome, Italy.

Silvia Lamonica (S)

Institute of Clinical Infectious Diseases, Catholic University of Sacred Heart, Policlinico Gemelli, Rome, Italy.

Francesca Montagnani (F)

Infectious Diseases Unit, Siena University Hospital, Viale Mario Bracci, 53100, Siena, Italy.

Elena Visconti (E)

Institute of Clinical Infectious Diseases, Catholic University of Sacred Heart, Policlinico Gemelli, Rome, Italy.

Andrea De Luca (A)

Infectious Diseases Unit, Siena University Hospital, Viale Mario Bracci, 53100, Siena, Italy. andrea.deluca@unisi.it.

Simona Di Giambenedetto (S)

Institute of Clinical Infectious Diseases, Catholic University of Sacred Heart, Policlinico Gemelli, Rome, Italy.

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Classifications MeSH

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questionsmedicales.fr Actions chimiques et utilisations Actions pharmacologiques Utilisations thérapeutiques Anti-infectieux Antiviraux Antirétroviraux Agents antiVIH Efficacy and tolerability of lamivudine plus...
questionsmedicales.fr Thérapeutique Traitement médicamenteux Association de médicaments Thérapie antirétrovirale hautement active Efficacy and tolerability of lamivudine plus...
questionsmedicales.fr Acides aminés, peptides et protéines Peptides Oligopeptides Sulfate d'atazanavir Efficacy and tolerability of lamivudine plus...
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questionsmedicales.fr Thérapeutique Traitement médicamenteux Association de médicaments Efficacy and tolerability of lamivudine plus...
questionsmedicales.fr Maladies du système immunitaire Déficits immunitaires Infections à VIH Efficacy and tolerability of lamivudine plus...
questionsmedicales.fr Maladies du système immunitaire Déficits immunitaires Infections à VIH Séropositivité VIH Efficacy and tolerability of lamivudine plus...
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