The purpose of this trial is to determine whether providing women with a weekly oral supplement of vitamin A, either preformed or as beta-carotene, at a dosage equivalent to a recommended intake from early pregnancy through three months postpartum, can reduce the risk of maternal mortality, fetal loss, or infant mortality.
Maternal mortality and vitamin A deficiency coexist in rural South Asia. In Nepal, weekly supplementation with vitamin A or beta-carotene during the child-bearing years reduced all-cause maternal mortality and, in night blind women, also infant mortality. The present trial is testing the efficacy of the same supplements from \~9 weeks' gestation to 12 weeks postpartum. The planned sample size is 68,000 pregnancies. It is being conducted in 19 rural unions, covering an area of \~750 sq km with a population of \~580,000 in Gaibandha and Southern Rangpur Districts in Northern Bangladesh. The study area was mapped as 596 "sectors" (unit of randomization), each comprising 200-275 households; \~135,000 houses were numerically addressed and, at the outset, 103,000 women were listed. Women are visited at home every 5 weeks by 596 trained female staff to detect pregnancy by a combination of menstrual history and urine testing. Newly married women are prospectively enlisted for pregnancy surveillance. Following informed consent urine-positive (pregnant) women detected during surveillance are enrolled to receive weekly a capsule containing 7000 retinol equivalents of preformed vitamin A, 42 mg of beta-carotene or placebo. Vital events are recorded weekly through 3 months postpartum. Trained interviewers conduct maternal nutritional and health and household socioeconomic assessments in the 1st trimester. At 3 months postpartum, interviewers assess both mother and infant for health and nutritional status, including apparent birth defects that are later physician-confirmed. An additional home health assessment occurs at 6 months post partum, and vital status is recorded for mother and infant at one year postpartum. A \~3% subsample of enrolled pregnant women participate in a substudy involving enhanced clinical, anthropometric, biochemical, body compositional, morbidity and interview-based assessment protocols in the 1st, 2nd and 3rd trimesters, and at 3 months post-partum. Reported maternal and infant deaths are verified and causes ascertained during "verbal autopsy" interviews with family members of the deceased.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
weekly dosage of either 7000 µg retinol equivalents as preformed vitamin A or 42 mg of beta-carotene from 1st trimester of pregnancy through 12 weeks after termination of pregnancy
Johns Hopkins School of Public Health
Baltimore, Maryland, United States
JiVitA Bangladesh Project
Rangpur, Rajshahi Division, Bangladesh
JiVitA Project Office
Rangpur City, Rangpur District, Bangladesh
All-cause, Pregnancy-related Mortality
Mortality evaluated on intent-to-treat basis
Time frame: Deaths during pregnancy through 12 weeks postpartum
All-cause 3-month Infant Mortality
Time frame: Deaths through the 1st 12 weeks of life
Maternal Morbidity, Including Obstetric Complications
Time frame: through the 1st 24 weeks following termination of pregnancy
Gestational Age at Birth
Time frame: within 24 weeks after birth
Fetal Growth and Postnatal Infant Growth Through Three Months of Age
Time frame: through the 1st 12 weeks after birth
Infant Morbidity Through 3 Months of Age
Time frame: within 24 weeks after birth
Plasma Beta-carotene in the Third Trimester of Pregnancy(Nutritonal Status of the Mother)
Time frame: Third trimester of pregnancy (about the 32nd week of gesatation)
Plasma Retinol at the Third Trimester of Pregnancy (Nutritional Status of the Mother)
Time frame: Third trimester of pregnancy (about the 32nd week of gestation)
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Purpose
PREVENTION
Masking
TRIPLE
Enrollment
59,666