Transmitted drug resistance, selection of resistance mutations and moderate antiretroviral efficacy in HIV-2: analysis of the HIV-2 Belgium and Luxembourg database.

BACKGROUND: Guidelines established for the treatment of HIV-1 infection and genotype interpretation do not apply for HIV-2. Data about antiretroviral (ARV) drug efficacy and resistance mutations is scarce. METHODS: Clinical data about HIV-2 infected patients in Belgium and Luxembourg were collected and the effect of ARV therapy on plasma viral load and CD4 counts were analysed. Viral RNA encoding for protease (PR) and reverse transcriptase (RT) from ARV-naïve and treated patients were sequenced. RESULTS: Sixty-five HIV-2 infected patients were included in this cohort. Twenty patients were tre... Mehr ...

Verfasser: Ruelle, Jean
Roman, François
Vandenbroucke, Anne-Thérèse
Lambert, Christine
Fransen, Katrien
Echahidi, Fedoua
Piérard, Denis
Verhofstede, Chris
Van Laethem, Kristel
Delforge, Marie-Luce
Vaira, Dolorès
Schmit, Jean-Claude
Goubau, Patrick
Dokumenttyp: Artikel
Erscheinungsdatum: 2008
Verlag/Hrsg.: BioMed Central Ltd.
Schlagwörter: Viral Load / Registries / RNA / Viral / Polymerase Chain Reaction / Mutation / Molecular Sequence Data / Middle Aged / Male / Luxembourg / Humans / HIV-2 / HIV Reverse Transcriptase / HIV Protease / HIV Infections / Genotype / Female / Drug Resistance / Multiple / Cohort Studies / CD4 Lymphocyte Count / Belgium / Anti-Retroviral Agents / Aged / Africa / Western / Adult
Sprache: Englisch
Permalink: https://search.fid-benelux.de/Record/base-29359657
Datenquelle: BASE; Originalkatalog
Powered By: BASE
Link(s) : http://hdl.handle.net/2078.1/11304

BACKGROUND: Guidelines established for the treatment of HIV-1 infection and genotype interpretation do not apply for HIV-2. Data about antiretroviral (ARV) drug efficacy and resistance mutations is scarce. METHODS: Clinical data about HIV-2 infected patients in Belgium and Luxembourg were collected and the effect of ARV therapy on plasma viral load and CD4 counts were analysed. Viral RNA encoding for protease (PR) and reverse transcriptase (RT) from ARV-naïve and treated patients were sequenced. RESULTS: Sixty-five HIV-2 infected patients were included in this cohort. Twenty patients were treated with 25 different ARV combinations in a total of 34 regimens and six months after the start of ARV therapy, only one third achieved viral load suppression. All of these successful regimens bar one contained protease inhibitors (PIs). Mean CD4 gains in the group of viral load suppressors and the group of patients treated with PI-containing regimens were respectively significantly higher than in the group of non-suppressors and the group of PI-sparing regimens. The most frequent mutations selected under therapy (compared to HIV-2 ROD) were V71I, L90M and I89V within PR. Within RT, they were M184V, Q151M, V111I and K65R. All of these mutations, except K65R and M184V, were also found in variable proportions in ARV-naïve patients. CONCLUSION: Despite a high rate of ARV treatment failure, better virological and immunological results were achieved with PI-containing regimens. The analysis of polymorphic positions and HIV-2 specific mutations selected during therapy showed for the first time that transmission of drug resistant viruses has occurred in Belgium and Luxembourg. The high heterogeneity in ARV combinations reflects a lack of guidelines for the treatment of HIV-2 infection.