HIV Infections Clinical Trial
Official title:
GMB: Phase IV, Multicenter, Randomized, Open-Label Pilot Study of Truvada (TDF+FTC) or Emtricitabine (FTC) Alone Versus HAART Interruption in HIV-Infected Patients Who Need to Interrupt HAART and Who Are Infected With HIV Isolates Containing at Least 2 TAMs (or K65R) and M184V
Many patients who already harbor drug-resistant HIV require interruption of HAART due to poor compliance, poor quality of life, toxicity or development of resistance. In these patients interruption of HAART has a negative impact on patient immune status due to the reemergence of wild-type virus which is in general more pathogenic than HIV isolates containing resistance mutations. There is a need for "bridging" antiretroviral regimens that might prolong time off conventional HAART whilst waiting for a new regimen that is either fully suppressive or less toxic or less demanding for the patient.
Virological failure associated with the appearance of resistant mutations is still common in
patients receiving HAART. When HAART fails patients and clinicians can chose from three
different courses of action:
1. Switch therapy to a new salvage regimen based on the results of resistance testing.
Success of the new salvage regimen is maximized if the new regimen includes
antiretroviral drugs without cross-resistance with previous failed drugs or,
preferably,new classes of drugs. In general, rescue regimens are more complicated for
patients due to its higher pill burden; more frequent dosing and sometimes need for
parenteral therapy (Enfuvirtide).
2. Stop therapy. This strategy is feasible in patient with relatively preserved immune
function. Time off antiretroviral therapy would be highly dependent on previous nadir
CD4 cell count (the lowest the nadir, the more rapidly patients loses CD4 cells). In
patients with multidrug resistant virus this strategy is used with the goal of
achieving virus reversion towards wild-type forms. Reversion towards wild-type virus
would theoretically "resensitize" HIV to prior failed drugs. Unfortunately, a number of
investigations have suggested that the loss of CD4 cell count occurred during the time
off therapy might not be regained after starting rescue therapy. In addition, reversion
towards wild type virus does not appear to be associated with a more favourable outcome
of rescue therapy.
3. Maintain failing therapy. This strategy has the potential advantage of decreasing the
rate of CD4 cell loss. It is known that certain mutations of HIV decrease viral fitness
and produce a less pathogenic virus. Consequently, compared to wild-type virus, CD4
destruction is decreased in the presence of resistance mutations. The very important
risk inherent to this strategy is the accumulation of new antiretroviral mutations if
the regimen is maintained. Due to cross-resistance among antiretroviral drugs,
accumulation of new mutations decreases the chances of success of a new salvage
regimen.
Choosing among these three different strategies depends on a number of important factors.
1. Availability of antiretroviral drugs active against resistant HIV isolates. Clinicians
would be more prone to switch to a new salvage regimen if the new regimen contains a
new class of drugs and/or at least three drugs without cross resistance with the
antiretroviral included in the failing regimen. This scenario is very likely after
first or second regimen failure. However, after third regimen failure the possibilities
of including at least three active drugs dramatically decrease. For deep salvage the
possibilities of constructing a viable rescue regimen often depends on enrolling the
patient in a clinical trial of a new antiretroviral (for example CCR5 inhibitors).
Enrolment in the trial very often implies that patients have to wait for an undefined
period of time until the trial starts.
2. Willingness of patient to switch to a more complicated regimen. After second regimen
failure, rescue therapies involve a higher pill burden, more frequent dosing and, in a
substantial number of cases, the need of parenteral therapy with enfuvirtide. In this
situation it is possible that the patient prefer not to start the new therapy due to
the negative impact of the new regimen in his quality of life.
3. Immune status of the patient. In patients with low CD4 cell count stopping therapy can
put the patient at risk of developing an opportunistic disease. In general patients and
clinicians are reluctant to stop therapy if the current CD4 cell count is below 200-250
cells/mL.
Apart from the setting of virological failure HAART interruption might be needed in patients
with well controlled viral replication (HIV viremia persistently below 50 copies/ mL).
Possible reasons for HAART interruption in this scenario are:
1. Toxicity of current regimen.
2. Patient desire (for example travel abroad).
3. Poor quality of life related to treatment issues.
4. Poor adherence to current HAART regimen and an impending risk of developing resistance
mutations. When a patient stop HAART due to these reasons, wild-type HIV re-emerges
with the consequent loss of CD4 cells. Depending on the immune status of the patient
and prior CD4 cell nadir time off therapy might be quite limited.
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Allocation: Randomized, Endpoint Classification: Safety Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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