HIV Clinical Trial
Official title:
Evaluation of Dolutegravir Interactions With Artemether-Lumefantrine and Amodiaquine-Artesunate
Malaria and HIV are found in the same regions of the world and developing countries are most affected by both diseases. For malaria, new drugs have been introduced called ACTs. These drugs are effective against malaria but little is known about how the levels of these drugs in blood relate to how effective these drugs are. For HIV, a new drug has been developed called dolutegravir which has potential to be widely used in developing countries. This proposal will explore how dolutegravir affects the drug levels of these antimalarial drugs and vice versa. In total, 46 healthy volunteers will participate in this study.
More than 90% of the malaria occurs in sub-Saharan Africa (WHO 2008), the region bearing 67%
of the global HIV burden (WHO 2011). Given the extensive overlap in geographical
distribution of these diseases, interactions between them could have profound public health
consequences. Significant biological interactions exist between HIV and malaria. HIV is
known to increase susceptibility to malaria infection (Whitworth, Morgan et al. 2000),
compromise the host's ability to clear malaria parasites (characterised by higher parasite
densities) (Francesconi, Fabiani et al. 2001), increase the risk of symptomatic malaria and
contribute to malaria treatment failure (Hewitt, Steketee et al. 2006). In areas of unstable
transmission, malaria mortality is higher in HIV-positive individuals. Additionally,
placental malaria infection in HIV positive individuals is associated with higher perinatal
mortality, low birth weight and HIV transmission, and this effect is not attenuated in
subsequent pregnancies, in contrast with HIV-negative individuals. Conversely, malaria
infection has been shown to increase HIV viral load (Hoffman, Jere et al. 1999, Kublin,
Patnaik et al. 2005), with the potential for both accelerated HIV disease progression and
increased HIV transmission (Abu-Raddad, Patnaik et al. 2006).
As of September 2011, Uganda had 1.4 million people living with HIV/AIDS; of those with
clinically advanced disease, 54% (313 117) were receiving ART (WHO). As southern African
countries are scaling up coverage of ART, they have also stepped up the fight against Pf
malaria by increasing the coverage of Insecticide Treated Nets and by adopting the use of
artemisinin-based combination therapies (ACTs) as first line treatment of malaria (USAID
2011). AL and AS-AQ are the most commonly utilized regimens in sub-Saharan Africa for first
line treatment for malaria (WHO 2008).
As a consequence of high rates of HIV-malaria co-infection and increasing availability of
both ACTs and ART in southern Africa, progressively more co-infected people will receive
both classes of drugs. However, the pharmacokinetics, safety and/or efficacy of ACTs such as
AL, AS-AQ and DHA-piperaquine in HIV-infected individuals who are on ART are poorly
understood. Many efficacy studies conducted as part of the drug development process of ACTs
have either not assessed the HIV status of study participants or systematically excluded
HIV-infected individuals. Few studies have systematically evaluated for potential drug-drug
interactions in a healthy volunteer setting.
Study Design
Open label, fixed sequence healthy volunteer study to compare pharmacokinetic interactions
between DTG and AL (Study A; crossover design), or AS-AQ (Study B; parallel group design).
Whilst a cross-over study design would be theoretically ideal for investigating both ACTs in
combination with DTG, desethylamodiaquine, an active metabolite of AQ has an extensive
terminal t1/2 of approximately 10 days; therefore it is not considered feasible to undertake
a cross-over design for this arm of the study, since the washout period between the two
phases would exceed two months, risking subject attrition. Furthermore, during that time
period, intercurrent illnesses and other important changes may occur within a subject,
leading changes in eligibility for the study. Therefore, two study designs are planned as
detailed in the Study Design Section.
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Allocation: Randomized, Endpoint Classification: Pharmacokinetics Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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