HIV Infections Clinical Trial
Official title:
The HIV Second-line Therapy AntiRetroviral Study in Patients Who Failed NNRTI-based Regimens
To evaluate the efficacy and safety at 48 weeks between LPV/r monotherapy and 2 NRTIs + LPV/r
therapy in patients failing a standard NNRTI-based treatment regimen. Also, to evaluate the
short-term 24-week efficacy and safety of Lopinavir/ritonavir (LPV/r) monotherapy and 2
NRTIs+LPV/r therapy in patients failing a standard NNRTI-based treatment regimen as an
interim analyses when 50% of the patients in each arm have reached 24 weeks after
randomization. Last, to define risk factors for monotherapy failure in HIV-treated
individuals
Hypothesis. The rate of virologic suppression is not inferior in the monotherapy arm.
With at least 80,000 HIV-1 infected individuals throughout Thailand currently on generically
produced fixed dose combination of d4T/3TC/NVP or GPOvir as a first line national
recommendation therapy, we will inevitably face with resistance problem in a large number of
patients near future. Therefore a comprehensive investigation into the best second line
regimen for these individuals is needed. Given the situation in Thailand where economic
burden is a major challenge, the second line regimen will have to offer the greatest possible
efficacy, and cost-effectiveness.
Second-line therapies necessitate treatment with combinations of drugs including protease
inhibitors[3]. Such high drug concentrations can be achieved by combining protease inhibitors
(such as indinavir, saquinavir, amprenavir and lopinavir) with ritonavir (RTV), known to
boost the other protease plasma levels through potent inhibition of the cytochrome P450. Low
dose RTV (100mg bid) significantly improves pharmacokinetics (AUC and plasma half life) of
most protease inhibitors with the exception of nelfinavir. However, these combinations are
more expensive, particularly if NRTIs are continued. In addition to increasing cost,
continuing NRTIs may not add to the antiviral effect (if resistance is present) and may
prolong the toxicity observed during the previous regimen.
Mono boosted PI therapy trials in HIV adults, as maintenance therapy after suppressed viral
load, have been shown to be effective and safe [4-6]. This strategy not only decreases number
of pill per dose but also saves ARV cost and might improve patient's adherence.
Lopinavir/ritonavir (LPV/r) is widely used protease inhibitor because of its high efficacy
and high genetic barrier. As maintenance monotherapy after HIV-1 viral suppression, LPV/r has
shown efficacy in 4 adult trials with 81-94% virological suppression[4, 7]. In the OK
study[4], the virological failure cases had significantly higher missed doses (p = 0.008).
Viral re-suppression after reintroduction of 2NRTIs was achieved in the LPV/r monotherapy
arm. A pilot study of switch to LPV/r monotherapy from NNRTI-based therapy was reported with
92% participants on treatment at week 48 having HIV RNA <75 copies/mL[8].
In the OK04 study[9], 196 patients were randomized to eitherLPV/r monotherapy or LPV/r plus
2NRTIs. The percentage of viral suppression to < 50 copies/ml, at week 96 was 77% in the
LPV/r monotherapy arm and 78% in the LPV/r plus 2NRTIs arm.
In the MONARK study, LPV/r monotherapy was used in 138 naïve adults and the percentage of
viral suppression at week 48 was 71% compared to 75% in the LPV/r plus AZT and 3TC arm[10] (p
= 0.69). Two patients in LPV/r monotherapy developed PI mutations but both were able to
resuppress HIV-RNA when NRTIs were added. Neither patient displayed phenotypic resistance to
LPV/r.
Therefore, we propose this comprehensive study to guide us in identifying the best second
line regimen in order to prepare for the large scale antiretroviral resistance problem in
Thailand.
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