HIV Clinical Trial
Official title:
Effect of Moringa Oleifera (Moringa, Drumstick/Horseradish Tree) on The Pharmacokinetics of Efavirenz and Nevirapine In-vivo.
A study will be conducted by scientists from the University of Zimbabwe to determine if
antiretroviral drugs are affected by taking herbs at the same time. This is important because
herbal medicines may interact with modern medicine to increase or decrease the amount of
medication in the body.
The drugs nevirapine and efavirenz will be studied. Both drugs are routinely used as part of
combination therapy for treating HIV. In this study it will be determined whether the
concentrations of the antiretroviral drugs nevirapine and efavirenz are low, high or are in
the desired range when taken together with the herb moringa.
The use of herbal supplements is widespread in Africa, particularly for the management of HIV
and AIDS. In Zimbabwe, the prevalence of herbal medicine use in HIV-infected people is as
high as 79% (Sebit et al., 2000). Several studies have shown that the herb Moringa oleifera
is among the top 10 herbs most commonly used by HIV-positive people in Zimbabwe (Makomeya et
al 2004, Monera et al 2008). Another review also cited Moringa as one of the 53 most
important African medicinal plants presently traded (van den Bout-van den Beukel et al 2006).
Others included Hypoxis hemerocallidea (African potato) and Sutherlandia frutescens-(Cancer
bush). Moringa is rich in β-carotene, protein, vitamin C, calcium and potassium and act as a
good source of natural antioxidants (Anwar et al.,2007).It is recommended by non-governmental
organisations and some African governments as an immune booster and a nutritional supplement
for people living with HIV and AIDS (Ncube, 2006). Most advocates and users believe that
since the herb is natural, it is free from all side effects and interactions.
Concomitant use of herbs with conventional drugs may lead to herb-drug interactions in the
same way that two or more co-administered drugs may interact. Herbal constituents that are
substrates for the same enzymes or transporters of conventional drugs may induce or inhibit
the enzymes and/or transporter activity. Pharmacokinetic endpoints such as area under the
curve (AUC), time to maximum plasma concentration (tmax), peak plasma concentration (Cmax),
trough concentration (Cmin), clearance (CL), volume of distribution (Vd/F) and half-life
(T1/2) may be altered significantly resulting in toxicity, more severe adverse effects,
sub-therapeutic drug concentrations, HIV resistance and treatment failure.The risk of
interaction increases as the number of co-administered drugs increases (de Maat et al 2003).
As a result, people taking herbal medicines while on antiretroviral therapy are at very high
risk because of the multitude use of highly active antiretroviral drugs and treatment of
opportunistic infections, and also because herbs contain a wide range of bioactive chemical
constituents.
However, evidence based information of such effects is usually lacking and as such; health
practitioners' ability to make relevant clinical decisions is limited. Results of a review of
in vitro studies suggest a need for in vivo metabolic drug-drug interaction studies (van den
Bout-van den Beukel et al 2006). Preliminary in vivo studies in animal models can serve as a
basis for clinical trials, the results of which are considered the gold standard in this era
of evidence-based medicine.
Primary objectives
1. To compare the steady-state pharmacokinetics of nevirapine and efavirenz in HIV-positive
patients before and after supplementation with Moringa oleifera leaf powder
2. To compare the single dose pharmacokinetics of nevirapine and efavirenz in rat models
before and after supplementation with Moringa oleifera leaf powder
Secondary objectives
3. To determine the bioavailability of Moringa oleifera leaf powder in humans after oral
dosing using beta carotene as a bio marker.
4. To compare urine chemistries and liver function tests in HIV patients before and after
supplementation with Moringa oleifera leaf powder
5. To determine the presence of any genetic variation in the participants in the genes that
code for CYP3A4 and CYP2B6
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