More than 3 billion people worldwide are at risk of acquiring malaria and pregnant women living with HIV in Africa are at particular risk. An effective prophylaxis regimen capable of preventing malaria and other common perinatal infections would have great potential to improve adverse birth outcomes. The purpose of this randomized controlled trial is to evaluate a new combination prophylaxis regimen in pregnant women with HIV in Cameroon to determine its efficacy and safety.
The World Health Organization (WHO) recommends malaria prophylaxis for all pregnant women living in endemic areas in order to reduce maternal anemia, low birth weight and perinatal mortality by 25-45%. The most commonly used regimen is intermittently dosed sulfadoxine-pyrimethamine (SP).Unfortunately, SP prophylaxis is contraindicated for HIV-infected pregnant women since co-administration with TMPS (trimethoprim-sulfamethoxazole) causes serious adverse events. TMPS (Bactrim or Cotrimoxazole) is an effective, well-tolerated, low-cost antibiotic that is used as prophylaxis in HIV-patients with low CD4 counts. It has anti-malarial activity with prophylactic efficacy that is comparable to SP (30-90%). Daily TMPS is recommended as malaria prophylaxis in pregnant women with HIV in many African countries (including Cameroon) but malaria infection rates are high even when medication compliance is excellent; thus, new and improved options are urgently needed. Azithromycin (AZ) is a macrolide antibiotic with activity against malaria, a good safety profile in pregnancy and proven utility as a part of combination malaria prevention regimens (such as SP-AZ). It also has activity against sexually transmitted infections (STI) and perinatal pathogens, including chlamydia (CT), gonorrhea (GC), syphilis and GBS (Streptococcus agalactiae or Group B Streptococcus), a potential but understudied contributor to high rates of newborn sepsis and death in Africa. SP-AZ prophylaxis in HIV-uninfected pregnant women has been reported to reduce prevalence of low birth weight (RR 0.74, 95% confidence interval (CI) 0.6-0.9) and preterm delivery (RR 0.66, 95% CI 0.48-0.91) compared to SP alone. Thus, the central hypothesis is that a TMPS-AZ combination will be more effective than standard TMPS malaria prophylaxis in pregnant women with HIV, and that it will also decrease STI coinfection. Investigators plan a test-of-concept of the central hypothesis by conducting a double blinded, Phase II randomized controlled trial (RCT).
Study Type
INTERVENTIONAL
Allocation
2 tabs po daily x 3 days at enrollment and at each monthly follow up visit
2 tabs po daily x 3 days at enrollment and at each monthly follow up visit
University of Alabama at Birmingham
Birmingham, Alabama, United States
Plasmodium Falciparum Peripheral Parasitemia
P. falciparum detected by microscopy or polymerase chain reaction (PCR)
Time frame: At end of pregnancy (>35 weeks) or at delivery
Proportion With Composite STI Outcome
Including chlamydia (NAAT (nucleic acid amplification test) positive) , gonorrhea (NAAT positive), syphilis (non-treponemal and treponemal test positive) infections.
Time frame: will be measured in both groups (>35 weeks) or at delivery
Low Birthweight (<2500 Grams)
Neonatal weight measured with digital scale
Time frame: at birth
Proportion With Adverse Birth Outcomes
Composite measure: low infant birthweight (\<2500 grams), miscarriage (\<28 weeks), preterm delivery (\<37 weeks), small for gestational age (SGA), congenital anomaly detected on surface examination, early neonatal mortality (within 7 days of birth)
Time frame: Birth outcomes will be measured at birth for all outcomes except early neonatal mortality defined as within 7 days of birth. Early neonatal mortality will be assessed at a six week follow up phone call.
Maternal Adherence to the Prophylactic Regimen
Directly observed therapy (DOT) in clinic for the 1st dose of study medication. Self-report and pill count will be used to assess adherence and maternal tolerability for study medications taken at home from the time of enrollment until delivery. At each follow up visit and at delivery, participants will complete a medication adherence survey. They will self-report adherence to the 3 day study regimen (AZ or placebo).
Time frame: Adherence of study medication taken at home will be documented from the date of randomization until the time of delivery, assessed up to 42 weeks.
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RANDOMIZED
Purpose
PREVENTION
Masking
QUADRUPLE
Enrollment
308
Proportion of Participants With Symptomatic Malaria
Fever and positive malaria test (rapid diagnostic test) at routine visits or sick call visits or maternal report of malaria diagnosis.
Time frame: From the date of randomization until the time of delivery, assessed up to 42 weeks.
Proportion With Placental Malaria
Placentas will be collected on a subset of women and impression smear will be used to assess for malaria infection
Time frame: At delivery
Proportion With Maternal Anemia and Severe Maternal Anemia
anemia defined as hemoglobin \<11 g/dL, severe anemia defined as hemoglobin \<7 g/dL.
Time frame: At the end of pregnancy (>35 weeks) or at delivery
Composite STI Measure (Including All STI Tests)
Proportion of women with GC/CT (by NAAT), syphilis (by serology), Mycoplasma genitalium (NAAT).
Time frame: After 35 weeks GA or at delivery
GBS Colonization
anogenital GBS colonization detected by NAAT (PCR)
Time frame: at or near term or at delivery