HIV Infections Clinical Trial
Official title:
Pharmacokinetics of Tenofovir and Tenofovir-diphosphate, Emtricitabine and Emtricitabine-triphosphate, and Efavirenz Once Daily Over 10 Days Following Drug Intake Cessation in Healthy Volunteers
The purpose of the study is to look at the levels of three HIV medications: tenofovir,
emtricitabine, and efavirenz in blood after the drug intake has been stopped in order to
understand how long these drugs persist in the blood. The study will specifically look at
blood levels of these three drugs (taken as a 3-in-1 tablet) after taking them every day for
14 days.
This study is not randomised which means that all subjects will receive all study
medications in the same order. You and the study doctor will know which study medications
you are taking at all times during the study.
The administration of combination antiretroviral therapy (cART) to HIV-infected patients has
been associated with a dramatic reduction in AIDS-related morbidity and mortality [1-3].
The key to successful HIV drug treatment is adhering to the prescribed combination every day
[2]. The approval of Atripla® (tenofovir/emtricitabine/efavirenz co-formulated in a single
tablet) provides HIV care providers with a "one tablet once a day" therapy, making adherence
much easier for patients.
However, in HIV therapy, successful adherence also means attention to intervals between
doses or dietary restrictions. Ideally, to guarantee long-term virological response,
HIV-infected patients should take their cART every day at the same time. However, cART is
for life and doses can be forgotten or delayed.
Importantly, the 24-week 'Five-on-Two-off' (FOTO) study results were presented in November
2008; these showed that when HIV-infected patients stable (viral load < 50 copies/mL) on
Atripla® were randomised to continue treatment daily or to stop taking it at weekends, no
difference in maintenance of undetectable viral load was observed. Eighty percent in the
control arm and 83% in the 'weekend off' arm had a viral load < 50 copies/mL [4]. This
suggests that either the drugs' effects, or the drugs themselves, persist for a significant
time following drug intake cessation. However, the persistence time and the inter-individual
variability of this parameter for the components of Atripla® have not been clearly defined.
A drug's persistence in plasma or in cells depends on its half life. Long half-life
antiretroviral agents may allow for missed or delayed doses, if concentrations are
maintained at therapeutic levels until the next dose is taken. NRTI are pro-drugs and must
be activated by different phosphorilation steps to be effective against HIV. Intracellular
triphosphate (TP) metabolites have been shown to be characterized by long half lives.
However, data on drug persistence are limited and whether drug doses can be omitted and
dosing delayed is unknown.
Knowledge of the length of time the drug contained in the Atripla® formulation lasts would
increase the confidence of doctors in this combination.
Importantly, triple regimen persistence should be investigated in order to provide
information on the permissiveness (of forgotten or delayed doses) of the whole regimen
rather than one single agent. Due to the simplicity of administering Atripla®, a study
investigating the pharmacokinetic "forgiveness" of tenofovir and emtricitabine (in plasma
and intracellularly) and plasma efavirenz would be readily performed in healthy volunteers
and would provide information on how to advise HIV infected patients on delayed and missed
doses.
Rationale for the pharmacogenomics analysis
Pharmacogenetics holds promise in HIV treatment because of the complexity and potential
toxicity of multi antiretroviral drug therapies that are prescribed for long periods. Thus
far, few candidate genes have been examined for a limited number of allelic variants, but a
number of confirmed associations have already emerged.
From a public health perspective, as antiretroviral medications become increasingly
available to racially and ethnically diverse populations worldwide, understanding the
genetic structures of each population may allow us to anticipate the impact of adverse
responses, even in groups that were not represented in drug registration trials.
The existing literature on pharmacogenetic determinants of antiretroviral drug exposure,
drug toxicity, as well as genetic markers associated with the rate of disease progression
underline the recent advances which occurred in the past few years.
However, it is expected that larger-scale comprehensive genome approaches will profoundly
change the landscape of knowledge in the future. Additional studies are needed to assess the
implications for long-term responses to antiretroviral agents.
For this reason we plan to collect a single blood sample from each participant in our
intensive pharmacokinetic studies, such as this one, in order to be able to investigate the
association between genetic polymorphisms in drug disposition genes (such as those encoding
for cytochrome P450 isoenzymes or transmembrane transporters) and drug exposure. A candidate
gene approach will be utilised to examine loci of interest. This procedure will provide
potentially important information on genetic influences on plasma drug concentrations and
give insight into how to improve the management of HIV-infected patients by individualising
therapy. These studies will not be powered for genetic associations but will enable us to
build a data base of genotype-phenotype. Prospective genetic studies would need to be
planned based on these preliminary data.
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Endpoint Classification: Pharmacokinetics Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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