HIV Infections Clinical Trial
Official title:
Randomised and Prospective Clinical Study to Evaluate the Efficacy and Safety of Lopinavir/Ritonavir Monotherapy Versus Darunavir/Ritonavir Monotherapies as Simplification Switching Strategies of PI/NNRTI-Triple Therapy Based-Regimens
The purpose of this study is to determine the non-inferiority in the efficacy of DRV/r (900/100 mg) monotherapy at 48 weeks versus LPV/r (400/100 mg) as simplification strategy in subjects with sustained viral suppression on stable PI or NNRTI-antiretroviral regimens.
The pillar of the current standard of care for highly active antiretroviral therapies
(HAART) is the use of two nucleoside reverse transcriptase inhibitors (NRTIs).1 However,
these agents can inhibit the mitochondrial DNA polymerase gamma, causing mitochondrial
dysfunction, which, in turn, may cause NRTI-related adverse events such as peripheral
neuropathy, pancreatitis, liver disturbances, lipid profile abnormalities or lipoatrophy.2
As a result, strategies aimed to avoid the long term exposure to NRTIs and their toxicities
are desirable for the management of HIV-infected patients.
Monotherapy with protease inhibitors (PIs) as a simplification approach therapy after an
induction period with conventional antiretroviral treatment, appears to be of great utility
for minimizing mitochondrial toxicity because of NRTIs. This approach may also increase
patient adherence, reduce costs and preserve future treatment options. However, concerns
remain regarding compartmental HIV replication due to limited drug penetration into the
central nervous system, risk factors associated with monotherapy failure as well as the
extrapolation of results obtained in clinical trial settings to routine clinical practice,
are still not well known.
In this regard, there are reports that have suggested that lopinavir/ritonavir (LPV/r)
monotherapy may be an effective therapeutic option for treatment of HIV-1 infection in
antiretroviral-naïve patients. 5,6 Moreover, some studies report that despite LPV/r allows
CSF concentrations lower than plasma, its concentrations exceed levels that suppress
wild-type HIV replication.7,8,9 However other authors have reported that LPV/r monotherapy
results in suboptimal HIV suppression in the CSF compartment in approximately 10% of
cases.10
Darunavir is the last PI with activity against wild-type and PI-resistant HIV. In ARTEMIS
trial, DRV/r at doses of 800/100 mg once daily have demonstrated that it is non inferior and
statistically superior than LPV/r and it is an effective treatment option for antiretroviral
(ARV)-naïve patients. In this study, patients receiving once-daily DRV/r achieved high
durable virologic response rates, which were comparable in patients with less favourable
baseline characteristics or suboptimal adherence. In addition, they had a low
discontinuation rate due to virologic failure or adverse events or both, did not develop
protease inhibitor resistance upon failure, and had suitable drug exposure. 11,12
All these benefits, coupled with the higher genetic barrier, its favourable safety and
plasmatic pharmacokinetic profile of DRV/r, suggest that DRV/r has the potential to be an
excellent option for monotherapy simplification strategies.
The investigators propose a prospective and randomised clinical trial that compares the
efficacy, safety and tolerability of DRV/r 900/100 mg monotherapy once daily versus LPV/r
400/100 monotherapy twice daily as simplification strategy in HIV-infected patients with
stable NNRTI or PI-based antiretroviral regimen and sustained viral suppression.
Aside to the main goal of this project, the investigators are going to make use of the
samples obtained from the CSF at 48 weeks of follow-up (as representative of the viruses
replicating in the central nervous system) and genital tract and plasma at the different
time points. The investigators will compare the sequence population of those organs from the
different patients in order to state if viruses not found in plasma at one time point but
found in reservoirs can be found in blood when the infection advance.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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