HIV Infections Clinical Trial
Official title:
Comparison of the Steady State Pharmacokinetics of Nevirapine, Stavudine Plus Lamivudine in HIV Positive Ugandan Patients Taking Triomune 40 With the Pharmacokinetics of the Originator Products.
This study aims to compare the steady state pharmacokinetics of stavudine, lamivudine, and nevirapine in HIV positive Ugandan patients taking Triomune 40 with the pharmacokinetics of the originator products known as Viramune, Epivir and Zerit 40.
The introduction of combination antiretroviral therapy (ART) has revolutionised the
treatment of HIV/AIDS. ART has been associated with significant reductions in morbidity and
mortality mainly in wealthy countries and Brazil. ART which consists of a cocktail of at
least three different potent anti-HIV drugs, has now been adopted as the standard of care
for the management of HIV disease in developed countries.
The major constraint for widespread use of antiretrovirals (ARVs) in developing countries
has been the high cost of drug acquisition and associated monitoring tests. The drug
acquisition cost of innovator ARV ranges from €12,000 to €20,000 per patient per year. This
compares with an annual cost of 558,000 Ugandan shilling or €260 per patient per year for
Triomune, the most commonly generically manufactured ARV.
Triomune exists as two formulations, Triomune 40 and Triomune 30, both manufactured by Cipla
Mumbai, India. Both contain nevirapine 200mg and lamivudine 150mg, however the Triomune 40
contains stavudine 40mg and Triomune 30 contains stavudine 30mg. This allows for the fact
that persons weighing >60kg require a dose of stavudine 40mg and those weighing <60kg
require a dose of stavudine 30mg. Therefore in patients weighing >60kg Tiomune 40 is
prescribed, in patients <60kg Triomune 30 is prescribed. At the time of study design the
majority of patients attending the Infectious Diseases Institute, Mulago Hospital and
receiving ARV with Triomune were >60kg and therefore receiving Triomune 40.
The available pharmacokinetic data for Triomune is limited to a single dose study in healthy
Indian volunteers which was performed by the manufacturer of Triomune, Cipla Mumbai and only
one independent bioequivalence study on the steady state pharmacokinetic parameters of
Triomune in HIV infected patients in Malawi. Of concern in this study Triomune was found not
to be bioequivalent to the originator products with significantly higher d4T levels in the
patients on Triomune when compared to the originator product. In this study the patients
also reported more side-effects, principally peripheral neuropathy, when taking Triomune and
the authors postulated that this may have been a result of the higher d4T levels in these
patients. It was also noted that nevirapine levels were markedly higher in Malawians
compared to western subjects of same weight, possibly due to genetic metabolic differences.
The authors concluded that similar evaluation of drug exposure should be performed as these
medications are introduced to new populations.
A study in the Cameroon examined the clinical outcome of 60 patients treated with Triomune
over a 24 week period. This important study by Laurent et al. is the first published study
addressing the issue of the quality of generic drugs and, as he points out, there are no
clinical trials assessing the effectiveness, safety and quality of fixed dose combination
drugs in resource limited environments. The study does however have several limitations. As
the author himself acknowledges the sample size is small and therefore "not as powerful as a
controlled trial". There is no comparison group taking branded (proprietary) drugs. The
study time at 24 weeks is too short to satisfactorily assess the efficacy of these drugs-
the European medicines Agency (EMEA), the European drug regulatory authority, requires a
study period of 48 weeks for assessment of efficacy. Some major drug studies comparing
different drug combinations have seen no significant difference in viral load suppression at
24 weeks but marked differences at 48 weeks. Laurent et al. performed in vitro dissolution
testing on the drugs in their study; however this does not translate into bioequivalence.
There are no bioequivalence data in this study. The authors did measure plasma trough drug
levels at three time points as a measure of adherence but these measurements cannot be used
to confirm bioequivalence.
Comparison(s) Steady state levels of stavudine, lamvivudine and nevirapine in HIV positive
patients taking Triomune 40 for one month compared with the steady state levels of these
agents when the originator products Zerit 40, Epivir and Viramune have been taken for one
month, with patients acting as their own controls.
Pharmacogenomics
Pharmacogenomics is the study of the effect of genetic variation on drug disposition. It is
a growing area of research and there is emerging data to support genomic differences in
antiretroviral drug levels and related toxicity. There is increasing evidence that drug
disposition varies between ethnic groups. In some cases this is due to different expression
of the genes which encode the various components of the cytochrome system, in others it is
felt to be linked to the varying expression of the genes encoding drug transporters. There
is currently extremely limited data in this area relating to Africans. By storing blood
samples from subjects enrolled in pharmacokinetic studies such as this a large and unique
pharmacogenomic resource would be build up at Makerere University.
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Allocation: Randomized, Endpoint Classification: Bio-equivalence Study, Intervention Model: Crossover Assignment, Masking: Open Label, Primary Purpose: Treatment
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