The purpose of this study is to demonstrate the feasibility, acceptability, and preliminary effectiveness of a focal mass drug administration program for household members of pregnant women to protect against malaria in pregnancy.
The scientific objective of this pilot study is to demonstrate the feasibility, acceptability, and preliminary effectiveness of a focal mass drug administration program for household members of pregnant women to protect against Malaria in Pregnancy. The hypothesis is that eliminating the parasite reservoir within the household will provide a complementary layer of protection against Malaria in Pregnancy especially when access to care is limited and visits may be delayed or missed. Aim 1: Determine the feasibility and acceptability of a Focal Mass Drug Administration program with dihydroartemisinin-piperaquine as a novel component of the Malaria in Pregnancy prevention package. The study team will conduct an open-label, randomized pilot study at a primary health center in rural western Uganda. The household members of women presenting to their first antenatal Clinic visit will be randomized 1:1:1: to (i) control (ii) one-time Focal Mass Drug Administration, or (iii) monthly Focal Mass Drug Administration. Using an established implementation framework, the study team will assess process measures such as the proportion of household members reached, willingness to take Dihydroartemisinin Piperaquine, adherence to the course of treatment, and frequency of adverse events. Aim 2: Estimate the efficacy of Focal Mass Drug Administration to create a "safe zone" in the immediate home environment and ultimately prevent Malaria in Pregnancy. Using the study design outlined in Aim 1, The study team will follow participating pregnant women and associated households through delivery, including longitudinal assessments of P. falciparum infection. As a pilot study, the trial is deliberately not powered for statistical tests of significance, but The study team will measure the incidence of (i) clinical malaria, defined as the presence of typical symptoms (e.g., fever, lethargy) and a positive malaria rapid diagnostic test (Rapid Diagnostic Test), (ii) asymptomatic P. falciparum parasitemia and placental malaria by Polymerase Chain Reaction throughout pregnancy and (iii) the incidence of adverse birth outcomes (e.g., stillbirth, low birth weight). In addition, the study team will measure the prevalence of asymptomatic parasitemia in household members using Rapid Diagnostic Tests at three time points to estimate the effectiveness of Focal Mass Drug Administration at maintaining a parasite-free zone
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
PREVENTION
Masking
NONE
Enrollment
300
A single or monthly dose of Dihydroartemisinin Piperaquine based on weight will be taken orally.
Bugoye Level III Health Center
Kasese, Uganda
Percent of eligible household members receiving fMDA
Proportion of eligible household members that receive fMDA intervention according to dosing schedule (i.e., one time or monthly)
Time frame: Day 1 to study completion, generally 5 months
Percent of household members enrolled
Proportion of household members who consent to participate
Time frame: At enrollment visit (Day 1)
Refusal to receive fMDA
Proportion of eligible household members who decline any fMDA intervention
Time frame: Day 1 to study completion, generally 5 months
fMDA Adherence
Proportion of DP blister packs returned with all medication taken (i.e., pill counts)
Time frame: Day 1 to study completion, generally 5 months
P. falciparum parasitemia among household members
Prevalence of P. falciparum parasitemia among household members at three time points (enrollment, mid-point, delivery) as measured by malaria rapid diagnostic test
Time frame: Day 1 to study completion, generally 5 months
P. falciparum parasitemia among pregnant women
Prevalence of P. falciparum parasitemia as measured by RDT or PCR among women during any point in pregnancy
Time frame: Day 1 to study completion, generally 5 months
P. falciparum parasitemia in peripheral and placental blood at delivery
Prevalence of P. falciparum parasitemia in peripheral and placental blood at delivery as measured by PCR
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Time frame: At time of birth/delivery
Clinical malaria incidence among pregnant women
Incidence of clinical malaria among pregnant women, defined as the presence of acute febrile illness and a positive malaria rapid diagnostic test (RDT)
Time frame: Day 1 to study completion, generally 5 months
Maternal anemia
Change in prevalence of maternal anemia, defined as Hemoglobin \<11 g/dL among participants
Time frame: Day 1 to study completion, generally 5 months
Adverse birth outcomes
Composite of adverse events including spontaneous abortion, premature delivery (\<37 weeks gestation), stillbirth, and low birthweight
Time frame: Day 1 to study completion, generally 5 months
Co-occurrence of malaria parasitemia in mother and household members
Proportion of RDT+ individuals in each household stratified by parasitemia status of pregnant women at enrollment visit
Time frame: Day 1 to study completion, generally 5 months
Number of adverse reactions to DP
Number of dihydroartemisinin-piperaquine administrations that result in vomiting or other known side effects
Time frame: Day 1 to study completion, generally 5 months