HIV Infections Clinical Trial
Official title:
Lumefantrine Pharmacokinetics When Administered as a Fixed Dose Combination With Artemether in HIV Positive Patients on Lopinavir/Ritonavir
With the roll out of antiretroviral therapy (ARV) for HIV across sub-Saharan Africa an unprecedented number of people will be commencing lifelong therapy. Current estimates are that 5-6 million people in sub-Saharan Africa require ART. At the same time, the World Health Organization (WHO) Roll Back Malaria campaign is aggressively promoting the use of artemether/lumefantrine as first-line therapy for malaria in this setting. Many patients in this setting have already become resistant to first-line ARV and have moved onto lopinavir/ritonavir (Kaletra) based second-line regimens. Kaletra is a potent inhibitor of Cytochrome P450 3A4 (CYP 3A4), an enzyme responsible for the metabolism of many drugs which is found predominantly in the liver and the gut. Lumefantrine, and to a lesser extent artemether, is extensively metabolized by CYP 3A4. Therefore when given to a patient already taking Kaletra for HIV, it is likely that elevated levels of these drugs in the patient will result. There is some concern that lumefantrine may be cardiotoxic due to its structural similarity to halofantrine which is known to cause irregular heart rhythms. This has not been borne out as yet in any studies performed with lumefantrine, however it is not known what levels will be achieved in patients when it is administered with a protease inhibitor such as Kaletra. The WHO has not addressed this issue in any of its previous policy documents but has identified ARV-antimalarial drug interaction studies as a research priority. This single dose pharmacokinetic (PK) study aims to compare the levels of lumefantrine/artemether that result when it is given to a patient on Kaletra with patients not on any ARV. Data generated by this study will help address this important knowledge gap which has been identified by WHO and others as meriting urgent investigation.
In 2004 there were an estimated 40 million people living with HIV, 95% of whom live in the
developing world. It is estimated that 5-6 million of these require antiretroviral therapy
(ARV) now, and this number will continue to rise. At the recent G8 summit in Gleneagles,
Scotland, a unanimous commitment to Universal Access to ARV by 2010 was made. This will
result in an unprecedented number of individuals, predominantly in the developing world,
commencing lifelong therapy with ARV. Currently the recommended second-line therapy for ARV
is a combination of two nucleoside reverse-transcriptase inhibitors (NRTI) and a protease
inhibitor (PI). The most widely recommended PI at this time in sub-Saharan Africa is Kaletra
(Abbott Laboratories) which is a combination of lopinavir, a PI, and ritonavir, a PI that is
a potent enzyme inhibitor and acts as a pharmacokinetic enhancer for lopinavir. Although
Kaletra is highly effective in the treatment of HIV, it is a drug that has significant
potential for drug-drug interactions. These are largely due to ritonavir's, and to a lesser
extent lopinavir's, potent inhibition of Cytochrome P450 3A4 (CYP 3A4), which can result in
dramatically raised levels of any co-administered drug metabolised by this same route.
Unfortunately these same people are also the constant victims of the malaria pandemic. There
are at least 300 million acute cases of malaria each year globally, resulting in more than a
million deaths, 90% of which occur in Africa. Increasing resistance to anti-malarials such
as chloroquine, amodiaquine, fansidar, sulphadoxine-pyrimethamine (SP) in East and West
Africa has led the WHO to recommend artemether-lumefantrine (Coartem - Novartis) as
first-line therapy for malaria for adults and children. By 2004, fourteen countries in
sub-Saharan Africa had adopted this as official policy, with the WHO applying pressure on
the rest to follow as part of its Roll Back Malaria Campaign. The WHO's recommendations
however makes no specific reference to the use of artemether-lumefantrine in HIV positive
patients, particularly in patients who are being treated with ARV, although in it's document
"Malaria and HIV/AIDS Interactions and Implications: Conclusions of a Technical Consultation
Convened by WHO, 23-25 June, 2004" it states that "additional research on interactions
between antiretroviral and antimalarial drugs is urgently needed." Coartem is already being
used in sub-Saharan Africa as treatment for malaria in HIV-positive individuals on ARV, and
this trend is likely to continue given the lack of explicit guidelines on their concomitant
administration.
Lumefantrine and artemether are both extensively metabolized by CYP 3A4. To date, no data
exist with regard to the potential interactions of these drugs with PI. This gives rise for
concern, in particular in the case of lumefantrine, that patients administered both drugs
concurrently are likely to have elevated lumefantrine levels with potential for associated
toxicity. Lumefantrine, unlike its predecessor halofantrine, does not seem to prolong the QT
interval (which can lead to adverse cardiac events), however there is no data with regard to
the potential for adverse events when administered with PI. Given the unknown potential for
interactions when co-administered with PI, in association with the massive roll out that is
occurring of both these drugs across sub-Saharan Africa and their concomitant use in
patients, it is essential that these issues be addressed to inform policy as a matter of
urgency.
Preliminary or supportive data:
Artemether is metabolized via CYP 3A4 to dihydroartemisinin (although both compounds have
antimalarial activity, dihydroartemisinin has greater potency). Inhibition of CYP 3A4 would
reduce dihydroartemisinin but increase artemether and potentially increase the short
half-life of artemether (1 - 2 hours). The effects of PI and NNRTI are unclear.
Lumefantrine and halofantrine are extensively metabolized by CYP 3A4. Inhibition of
halofantrine metabolism could potentially prolong QT interval; given the narrow therapeutic
index of this drug, combination with PI is contraindicated and NVP and EFV should be used
with caution. Lumefantrine does not seem to prolong the QT interval and is much safer than
halofantrine. In a single-dose study in combination with ketoconazole, a potent inhibitor of
CYP 3A4, lumefantrine Cmax and AUC were doubled but no clinically significant QT effects
were noted. Nevertheless, the Novartis Drug Monograph for Coartem lists CYP 3A4 inhibitors,
including Ketoconazole and PI, under precautions/contraindications, despite stating in the
same document that "dose adjustment of coartemether appears to be unnecessary when
administered in association with ketoconazole or another potent inhibitor of CYP 3A4
activity." No studies however exist in the literature or are listed in the product monograph
addressing the important potential interaction with PI. The WHO and a recent editorial in
AIDS identify an urgent need for interaction data and state that studies should be
prioritized to address this gap in knowledge. Currently in practice, coartem is being
administered to patients in sub-Saharan Africa and WHO policy and guidelines do not address
this issue.
Significance of the study:
As outlined in the background, this study is of urgent public health importance in the
developing world where ARV and anti-malarials are used concomitantly. There are increasing
numbers of HIV patients in Uganda moving on to second-line therapy with Kaletra and these
are already being treated with coartem where they can afford it. The consequences of
prescribing these drugs concomitantly have not been elucidated. The WHO has made no
recommendations to guide treatment in this situation and there are no study data available
to guide policy. Data generated by this study would help address this important gap which
has been identified by WHO and others as meriting urgent investigation.
Hypothesis:
That administration of the lumefantrine and artemether-containing antimalarial combination
therapy (Coartem) to HIV-positive patients receiving lopinavir/ritonavir (Kaletra) results
in increased exposure to lumefantrine and/or artemether thus putting the patient at
increased risk of toxicity from these drugs.
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Allocation: Non-Randomized, Endpoint Classification: Pharmacokinetics Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Basic Science
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