Malaria Clinical Trial
Official title:
A Randomized Controlled Trial of Monthly Dihydroartemisinin-piperaquine Versus Monthly Sulfadoxine-pyrimethamine Versus Daily Trimethoprim-sulfamethoxazole Versus No Therapy for the Prevention of Malaria
Young African children living in high transmission areas suffer the greatest burden of malaria. In most African countries, such as Uganda, the only current preventive measure against malaria in high transmission settings is the use of insecticide treated bednets (ITNs). Preliminary data show that even in the setting of ITN use, young children living in a high transmission setting suffer almost 4 episodes of clinical malaria per year, highlighting the need for new preventive strategies. Chemopreventive strategies offer a potential means of reducing the burden of malaria among young children living in a high transmission setting. This study will compare the efficacy and safety of 3 promising chemopreventive strategies (monthly dihydroartemisinin-piperaquine, monthly sulfadoxine-pyrimethamine, daily trimethoprim-sulfamethoxazole) with the current standard of no chemoprevention and will be conducted in two distinct patient populations: 1) HIV-unexposed children (HIV-uninfected children born to HIV-uninfected mothers) and 2) HIV-exposed children (HIV-uninfected children born to HIV-infected mothers). The intervention will begin in HIV-unexposed children when they reach 6 months of age, the time at which the incidence of malaria begins to increase, and will be continued until the children reach 24 months of age, which prior data suggest is when the incidence of malaria begins to decline due to the development of semi-immunity. In addition, study participants will be followed for one additional year following chemopreventive therapy to examine for "rebound" in the incidence of malaria following our intervention. HIV-exposed children will begin the intervention when they have completed breastfeeding and have been confirmed to remain HIV-uninfected. The intervention will continue until study participants reach 24 months of age and then the study participants will be followed for an additional year to examine for rebound in the incidence of malaria. It is anticipated that the results of this study will provide valuable comparative data on the effect of different chemopreventive strategies on malaria incidence in two distinct patient populations at high risk for malaria. In addition it is anticipated the results of this study will provide insight into the development of naturally acquired antimalarial immunity in the setting of chemopreventive therapy that will differ in terms of the drug regimens, the age at which the intervention is started, and the HIV status of the mothers.
Convenience sampling will be used to enroll a cohort of 600 HIV-uninfected infants between
the ages of 4-5 months of age according to the following strata based on the mother's HIV
status: 1) 200 HIV-exposed infants born to HIV-infected mothers, and 2) 400 HIV-unexposed
infants born to HIV-uninfected mothers. Potential study participants will be identified from
the Tororo District Hospital Antenatal Clinic and surrounding clinics providing routine
pediatric care. Potential study participants less than 6 months of age and their
parents/guardians will be referred to our study clinic for screening. Eligible children will
be enrolled when they reach 4-5 months of age and followed until the age of 36 months for
all their routine medical care at our designated study clinic. All mother-child pairs will
receive 2 long lasting ITNs at enrollment and, as available, a basic care package including
a safe water vessel, multivitamins and condoms. HIV-unexposed children will be randomized to
one of four chemoprevention arms when they reach 6 months of age. All HIV-exposed children
born to HIV-infected mothers will be given TS prophylaxis and mothers will be encouraged to
introduce food at 6 months of life and continue breastfeeding until 1 year of life, in
accordance with Ugandan Ministry of Health (MOH) guidelines. HIV-exposed children will
retested for HIV approximately every 60 days during breastfeeding and 6 weeks following
cessation of breastfeeding. HIV-exposed children who remain HIV-uninfected following
cessation of breastfeeding will be randomized to one of four chemoprevention arms.
HIV-exposed children who test positive for HIV during the course of the study (those who
seroconvert during breastfeeding) will be excluded from the study and referred for
appropriate care.
During the follow-up period, all patients presenting to the clinic with a new episode of
fever will undergo standard evaluation (history, physical examination and Giemsa-stained
blood smear) for the diagnosis of malaria. Children diagnosed with uncomplicated malaria
will be treated with AL and children diagnosed with complicated malaria will be treated with
quinine in accordance with national guidelines. Response to antimalarial therapy will be
assessed using standardized guidelines. All AL treatment failures occurring within 14 days
of diagnosis will be treated with quinine in accordance with national guidelines. In the
event that a patient fails quinine therapy, therapy will be repeated with quinine plus
clindamycin. Patients with complicated malaria who have contraindications to giving quinine
will be treated with parenteral artesunate. All episodes diagnosed more than 14 days after a
previous episode will be considered new episodes for treatment purposes. After two years of
age, patients with uncomplicated malaria will have follow up visits on the days Antimalarial
drugs are administered only (Day 0, 1, and 2). Routine assessments will be performed in the
study clinic approximately every 30 days. Routine assessments will include review of study
protocol with parents/guardians of study participants, assessment for any outside medical
care, assessment for adherence to assigned chemopreventive therapy, a focused history and
physical examination and routine blood smears for the detection of asymptomatic parasitemia.
Routine phlebotomy will be performed approximately every 120 days for all study participants
for CBC, glucose and ALT measurements.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Prevention
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