Pharmacokinetics Clinical Trial
Official title:
Comparison of the Pharmacokinetics of Antiretroviral Agents in HIV Infected Ugandan Women During and After Pregnancy
In HIV-infected women, the use of combination therapy with antiretrovirals (ARV) in
pregnancy prevents HIV related morbidity and mortality and prevents mother-to-child
transmission of the HIV virus.
Specifically, suppression of the virus to an undetectable level is important during the
delivery of the baby to minimize potential HIV exposure. In Sub-Saharan Africa, the use of
ARV combinations containing nevirapine is the cornerstone of current HIV therapy, due to an
affordable cost, availability in a fixed dose combination pill, and generic availability.
Maintaining the efficacy and preventing development of resistance against this agent by the
HIV virus is imperative, as second line therapies are often more difficult to obtain, are
more expensive, and present more challenges in drug storage in clinics and in the community.
Pregnancy adds another dimension to the challenge of treating women with HIV, as the
physiologic and metabolic changes can affect levels of antiretroviral agents in the body.
Though these changes are known to exist, few trials have evaluated the effect of these
factors on the pharmacokinetics of antiretroviral agents and their impact has yet to be
demonstrated.
We wish to evaluate if the physiologic changes that occur during pregnancy impact the levels
of stavudine, lamivudine, and nevirapine compared to those of a non-pregnant, HIV-infected
Ugandan female. These data are imperative to ensure adequate suppression of the HIV virus
throughout pregnancy.
In HIV-infected women, the use of combination therapy with antiretrovirals (ARV) in
pregnancy prevents HIV related morbidity and mortality and prevents mother-to-child
transmission of the HIV virus.1 Specifically, suppression of the virus to an undetectable
level is important during the delivery of the baby to minimize potential HIV exposure.
Commonly prescribed ARV therapy in Ugandan pregnant women includes a combination of two
NRTIs, along with a non-nucleoside reverse transcriptase inhibitor (NNRTI), nevirapine. In
Sub-Saharan Africa, the use of nevirapine containing regimens is the cornerstone of current
ARV therapy, due to an affordable cost, availability in a fixed dose combination pill, and
generic availability. Maintaining the efficacy and preventing development of resistance
against this agent by the HIV virus is imperative, as second line therapies are often more
difficult to obtain, are more expensive, and present more challenges in drug storage in
clinics and in the community.
Data have demonstrated that higher exposure to nevirapine is associated with a greater
likelihood of achieving virologic control as well as maintaining virologic response over the
long term, while sub-optimal drug levels may result in the development of viral resistance.2
The use of combination therapy is important due to the development of resistance seen using
single dose therapy with nevirapine at delivery.3 Resistance to nevirapine is particularly
worrisome due to the cross-resistance between nevirapine and other NNRTIs, potentially
eliminating one essential class of ARVs used to treat HIV. Evaluating nevirapine exposure is
also important to avoid toxicities related to excess levels of nevirapine, which may
compromise patient adherence to the regimen and put the woman at risk for virologic failure
in addition to increased drug toxicity.4, 5
To our knowledge, most studies to date have only evaluated the pharmacokinetics of first
dose nevirapine in HIV-infected pregnant women during delivery.6,7 Other studies have had
too few sampling times to fully characterize the pharmacokinetic parameters of nevirapine.
However, previous studies have demonstrated that pharmacokinetic changes do occur with other
ARVs metabolized by a metabolic path similar to nevirapine. For example, one published study
demonstrated lower levels of nelfinavir and a disproportionate amount of the nelfinavir M8
metabolite in pregnant women during their third trimester, possibly implicating alterations
in the cytochrome P450 enzyme system responsible for both nelfinavir and nevirapine
metabolism.8, 9 Given this evidence with similarly metabolized drugs, it is important to
definitively characterize nevirapine pharmacokinetics to ensure the safe use of this drug
during pregnancy.
Data have also demonstrated a direct correlation between zidovudine intracellular
triphosphate concentrations and change in CD4 cell count during therapy as well as a direct
correlation between lamivudine intracellular triphosphate concentrations and decline in HIV
RNA in plasma.10 Data have also shown that there is a wide inter-patient variability in the
concentration of the NRTIs, and adjusting these concentrations based on therapeutic drug
monitoring has resulted in improved virologic outcomes for patients.11, 12 No information is
known about the intracellular triphosphorylated concentrations of the NRTIs in the pregnant
female. We seek to establish if there is a necessity for further evaluation of intracellular
levels of all NRTI agents in the pregnant population through this research.
The available pharmacokinetic data to date, have primarily evaluated male populations in the
western world. We are just beginning to understand the complex pharmacogenomic mechanisms
that play a role in pharmacokinetics and pharmacodynamics. Efavirenz, also an NNRTI, and
nevirapine have both been identified as having different pharmacokinetic properties in
African patients as compared to American, European, and South American patients.13,14 These
changes will play a significant role in the long term efficacy and toxicity of these agents
as they are used on a more widespread basis in Sub-Saharan Africa. Evaluating these changes
in African women during pregnancy is also essential as females represent the predominant
gender impacted by HIV in Sub-Saharan Africa. These changes during pregnancy may impact the
safety of these agents in pregnant females if the levels are higher than expected, and may
also impact the mother-to-child transmission rate and long term use of these agents if the
levels are lower than desired.
Pregnancy adds another dimension to the challenge of treating women with HIV, as the
physiologic and metabolic changes can impact the pharmacokinetics of antiretroviral agents.
Proposed mechanisms include absorption changes due to prolonged gastric and intestinal
emptying time, decreased gastric acid secretion, and increased mucus secretion; increased
volume of distribution of drug caused by increased total body water and fat, and decreased
plasma protein concentration; changes in elimination related to stimulation of hepatic
microsomal enzymes and inhibition of microsomal oxidases; the effects of the fetus including
compartmentalization of drugs in the fetus and placenta, biotransformation of drugs by the
fetus and placenta, and additional elimination of drugs by the fetus.15,16 Though these
physiologic and metabolic changes are known to exist, few trials have evaluated the effect
of these factors on the pharmacokinetics of antiretroviral agents and their impact has yet
to be demonstrated.
Few pharmacokinetic studies have been undertaken to date in Sub-Saharan Africa, though it is
becoming recognized that in order to support the antiretroviral rollout program, these
studies are essential for the safe and effective long-term use of these agents. The
University of Makerere, Infectious Diseases Institute, is establishing a strong foundation
for pharmacokinetic work to take place in Uganda through the development of a
pharmacokinetic laboratory which will become the leading resource for pharmacokinetic work
in Sub-Saharan Africa. This makes the Makerere University the logical location for this
essential evaluation. One of the first studies evaluating pharmacokinetic parameters in
African patients was performed by our co-investigators at the Joint Clinical Research Center
in Kampala, and established that pharmacokinetic evaluation of these drugs in an African
population is both necessary and logistically feasible(22) .
We wish to evaluate if the physiologic changes that occur during pregnancy impact the
pharmacokinetics of stavudine, lamivudine, and nevirapine compared to those of a
non-pregnant, HIV-infected Ugandan female. Evaluation of drug concentrations at steady
state, instead of after a single dose is essential, as most patients are maintained on these
medications throughout their pregnancy to ensure complete virologic suppression at the time
of delivery. These data are imperative to ensure adequate viral suppression throughout
pregnancy and to minimize the likelihood of the development of viral resistance engendered
by inadequate drug concentrations
;
Observational Model: Cohort, Time Perspective: Prospective
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