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Switch to LPV/r monotherapy
ARV-trial.com Switch to LPV/r monotherapy Pilot LPV/r M03-613 LPV/r Mono KalMo OK OK04 KALESOLO MOST HIV-NAT 077 1
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OK Study: Switch LPV/r + 2NRTIs to LPV/r monotherapy
Design Randomisation 1 : 1 Open-label W48 N = 21 LPV/r 400/100 mg bid + continuation of the 2 NRTIs 42 HIV+ ≥ 18 years On 2 NRTIs + LPV/r > 4 weeks No history of prior virologic failure on PI HIV-1 RNA < 50 c/mL > 6 months N = 21 LPV/r 400/100 mg bid Endpoints: pilot study Primary outcome: proportion of patients with HIV-1 RNA < 500 c/mL at W48 (ITT analysis) Secondary outcomes: proportion of patients with HIV-1 RNA < 50 c/mL at W48, time to loss of virologic suppression, development of HIV resistance, CD4 changes, safety, treatment-related adverse events OK Arribas J, JAIDS 2005;40:280-7
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OK Study: Switch LPV/r + 2NRTIs to LPV/r monotherapy
ARV-trial.com OK Study: Switch LPV/r + 2NRTIs to LPV/r monotherapy Baseline characteristics and patient disposition LPV/r + 2 NRTIs N = 21 LPV/r monotherapy Median age, years 42 Female 14% 19% IV drug user 29% 38% HCV co-infection 48% Prior AIDS 67% 71% CD4 cell count, median/mm3 585 662 HIV-RNA pre-HAART, median log10 c/mL 4.93 5.11 Time with HIV-1 RNA < 50 c/mL, median months 15.7 28.6 Months on LPV/r, median 13 N of PIs prior to LPV/r: 0 / 1 / 2 29% / 47% / 24% 33% / 67% / 0 NRTIs prior to randomisation ZDV + 3TC d4T + 3TC Other 43% 29% 33% Discontinuation by W48, n 1 (hyperlipidemia) 1 (lost to follow-up) OK Arribas J, JAIDS 2005;40:280-7
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OK Study: Switch LPV/r + 2NRTIs to LPV/r monotherapy
Virologic outcome HIV-1 RNA < 500 c/mL at W48 (ITT)* HIV-1 RNA < 50 c/mL at W72 (ITT) 25 50 100 75 95 81 123 % 90.5 129 127 N= 95% CI for the difference = ; 4.9 95% CI for the difference = ; 11.4 Time to loss of virologic suppression Percent with suppression 20 40 60 100 Weeks 80 12 24 36 48 * All patients with HIV RNA < 500 c/mL were < 50 c/mL LPV/r + 2 NRTIs LPV/r mono OK Arribas J, JAIDS 2005;40:280-7
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OK Study: Switch LPV/r + 2NRTIs to LPV/r monotherapy
Other outcomes 4 blips in the monotherapy group vs 1 in the triple therapy group No significant changes in CD4 cell count in any group at W48 Median adherence was 96% in the triple therapy group and 86% in the monotherapy group (p = 0.09) Loss of virologic suppression was associated with shorter time of HIV-1 RNA < 50 c/mL prior to monotherapy (median of 40 weeks vs 132 weeks in patients with maintenance of virologic suppression ; p = 0.02) Patients with loss of virologic suppression on LPV/r monotherapy were safely reinduced with prior NRTIs and achieved HIV-1 RNA < 50 c/mL Grade 3 hypertriglyceridemia occurred in 3 patients in the triple therapy arm vs none in the monotherapy arm. One patient in each arm had grade 3 hypercholesterolemia Conclusion: this pilot study provides preliminary evidence suggesting that in patients suppressed on a triple therapy with LPV/r, continuation with LPV/r monotherapy can maintain HIV suppression in a large proportion of patients OK Arribas J, JAIDS 2005;40:280-7
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