HIV Infections Clinical Trial
Official title:
A Multicenter, Randomized, Open Label, Clinical Trial Comparing a QD Regimen of Didanosine, Lamivudine and Efavirenz With a Standard BID Regimen of Zidovudine, Lamivudine and Efavirenz in the Starting Treatment of Human Immunodeficiency Virus Infection (GESIDA 39/03)
The purpose of this study is to compare the antiviral activity of two treatment groups for HIV chronic infection: a QD regimen of didanosine, lamivudine and efavirenz versus a BID regimen of zidovudine, lamivudine and efavirenz. Both will be administered with food in the starting treatment of human immunodeficiency virus infection at Week 48.
The inhibition of HIV replication mediated by HAART causes an actual immunological
reconstitution that has been clinically evidenced as a dramatic reduction in mortality,
incidence of opportunistic diseases, hospital admissions and costs associated with
healthcare in HIV-infected patients, which has been shown since the year 1996.
Unfortunately, the eradication of HIV is not feasible with the therapies available;
therefore, treatment of HIV infection is currently approached as a "life-long" strategy.
HAART is not free from middle and long-term adverse events.
It must be considered that, until relatively recently, the HAART regimens required taking a
high number of tablets several times daily, frequently with diet restrictions, which made
compliance difficult and improved the quality of life of the patients. In any case, it must
be noted that insufficient compliance with HAART can have harmful consequences for the
patient, public health and health resources.
The factors predicting compliance with ART can depend on the patient, the healthcare team
and the therapeutic regimen.
As mentioned above, until recent dates, HAART has gathered all factors making compliance
difficult: long-term duration, over one drug, over one dose daily and presence of adverse
events. Therefore, the adequate compliance is an actual challenge for patients and for the
health staff and has been considered, with a good criterion, the weak point of
antiretroviral treatment.
For all the above, it can be stated that the ideal HAART regimen would be that with few
tablets and that could be taken once daily. The expected advantages of QD regimens could
include mainly three: first, they will improve compliance, which will have a highly positive
effect on the antiviral efficacy of HAART. On the other hand, QD regimens will enable that
HAART is better adapted to the lifestyle of the patient and will have a low interference
with working hours, so they will be more convenient and improve quality of life. Finally, it
must be noted that QD regimens will enable for monitoring HAART directly, and will allow for
a relatively significant group of patients in our setting to follow the treatment with a
greater guarantee of success, such as those with problems of drug addiction, lack of social
support, mental disease and those admitted to penitentiary centers.
The main disadvantage of QD regimens is the virtual lack of large clinical trials comparing
this therapeutic approach to other potent, well-established BID regimens. Therefore, it is
very interesting to examine this approach in a randomized clinical trial with an adequate
design such as that proposed.
The second problem is the consequences that result of missing a dose since this could entail
that for some time - in the 24 hours following the failure - the drug concentrations could
decrease enough to stop inhibiting viral replication; this could also promote the emergence
of viral strains resistant to the drugs. In principle, the implications of missing a dose
depend substantially on the pharmacokinetic properties included in the QD regimen (Cmin,
half-life, intracellular concentrations, and the IC50 of the HIV of each patient), so that,
the higher the drug half-life and the higher the Cmin/IC50 ratio, the higher the probability
that alter missing a dose the Cmin persists above the IC50 of the HIV strain of the patient.
Therefore, it is important to select drugs with pharmacokinetic profiles and an antiviral
potency enough for QD administration (vide infra).
BID regimen (efavirenz + zidovudine + lamivudine):
In this study, we have chosen as BID regimen that containing NNRTI efavirenz (Sustiva®) and
Combivir® which is the commercial combination of the NRTI zidovudine + lamivudine, that will
lead patients to take one tablet in the morning and 2 tablets at night. We have chosen this
regimen (zidovudine + lamivudine + efavirenz) because it is the starting treatment regimen
for HIV chronic infection best studied and considered by many as the gold standard for this
indication.
QD regimen (efavirenz + didanosine + lamivudine):
The QD regimen will be made up by didanosine (capsule-CT) + lamivudine + efavirenz, a
regimen containing three tablets that must be taken together at night and which is the QD
regimen with most experience to date. We have chosen as combination of NRTI didanosine and
lamivudine, drugs authorized for QD use with a very good safety profile and no interactions
with each other and with efavirenz. The combination of didanosine and lamivudine is highly
attractive and is in fact recommended for the starting HAART by various agencies though not
at the same level as the combination of zidovudine and lamivudine (which can be only
administered BID) just because there are less randomized clinical trials with the former
than with the latter combination of NRTI. Therefore, one of the strengths of the study is
that it proposes the possibility of assessing the combination of didanosine and lamivudine
in a starting HAART regimen.
In this study, the patients allocated to the QD regimen containing didanosine (capsule-CT) +
lamivudine + efavirenz will take all tablets together at night with dinner. In principle,
this involves a minor deviation from the data sheet of didanosine where it is specified that
the drug must be taken fasting.
Didanosine is the second antiretroviral drug marketed and, in the last decade, the
presentation and dosage form of this drug have improved remarkably, from bags with buffered
powder for twice daily administration, with dispersible tablets with buffer, to the current
dosage form which is a gastroresistant capsule (capsule-CT) which allows for administration
in once daily doses and that, since it has no buffer, has improved substantially the gastric
tolerance to the drug.
The formulations of didanosine as powder or buffered dispersible tablets must be taken
fasting for absorption to be optimum, since its administration with food reduces
significantly drug absorption and plasma concentrations. However, the effect of food on the
absorption of capsules-CT does not cause an unequivocal reduction in drug exposure.
Primary Objective:
- To compare the antiviral activity of the two treatment groups (QD vs BID) at Week 48,
based on the percentage of patients with HIV-RNA levels <50 c/ml.
Secondary Objectives:
- To compare the percentage of patients responding to the treatment with HIV-RNA levels <
400 c/ml at Week 48, with the same approach of analysis as for the primary objective.
- To compare the time to therapy failure at Week 48 in both treatment regimens.
- To compare the increase in the CD4 cell levels from baseline to Week 48 in both
treatment regiments.
- To compare the impact on the quality of life of both treatment regimens.
- To compare compliance of both treatment regimens.
- To compare the safety and tolerance of both treatment regimens along the 48 weeks of
treatment.
- To assess the efficacy of the administration of didanosine together with food.
Randomization Procedure:
The randomization will be centralized and stratified by the baseline viral burden level,
being higher or lower than 100,000 cop/ml. The patients giving their written informed
consent will be included in the study. To include a patient, the clinical trial agency
Gesida will be contacted by phone.
Study Procedures:
HIV-RNA, CD4 and routine labs will be collected at screening, baseline, w1, w4, w12, w24 and
w48. Quality of life will be measured with a self-patient report questionnaire (MOS-HIV).
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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