Malaria Clinical Trial
Official title:
A Randomised, Placebo Controlled Trial of Intermittent Preventative Treatment With Sulfadoxine-pyrimethamine in Gambian Multigravidae.
Malaria is particularly harmful during pregnancy causing anemia in the mother and low birth weight which, in turn, increases infant mortality. Thus, the World Health Organization (WHO) now recommends that all pregnant women who live in malaria endemic areas of Africa should receive sulfadoxine-pyrimethamine (SP) at monthly intervals during the second and third trimesters of pregnancy. Malaria is especially severe during first pregnancies and the value of intermittent preventative treatment with SP during first pregnancies has been clearly shown. However, it is less certain whether multigravidae, who are at less risk, also benefit from intermittent preventative treatment with SP. To investigate this, a trial has been conducted in Gambian multigravidae who were given intermittent preventative treatment with SP or placebo during the second and third trimesters. The prevalence of anemia six weeks after delivery, low birth weight and poor outcome of pregnancy in women in each group were studied.
Objective
The objective of this study was to determine whether intermittent preventative treatment
(IPTp) with sulfadoxine-pyrimethamine (SP) reduced the prevalence of anemia and low birth
weight in Gambian multigravidae.
Study area
The study was carried out in 14 mother and child health (MCH) clinics situated on the north
and south banks of the River Gambia near to the town of Farafenni in the centre of the
country. In this area, malaria is highly seasonal with an entomological inoculation rate of
10 -50 infectious bites per year.
Study population
All women who attended one of the study clinics during the trial period and who were
multigravidae were asked if they wished to join the study. If this was the case, an initial
screening questionnaire was administered to assess their suitability to do so. Eligibility
criteria were - a pregnancy of more than 15 weeks gestation, a hemoglobin (Hb) concentration
of more than 7 g/dL, absence of a history of sensitivity to sulfonamides and absence of any
chronic underlying illness.
Randomisation
If a woman met the eligibility criteria, informed written consent was sought and, if this
was given, the woman was formally recruited to the study and allocated a trial number and
randomised to receive either SP or placebo. Randomisation was done in blocks of 12; each
field worker was assigned a number of blocks to ensure balanced recruitment between centers.
Drug administration
Women were allocated to receive SP (pyrimethamine 25 mg + sulfadoxine 500 mg)(Cosmos
Pharmaceuticals, Nairobi) or matching placebo. An initial dose of SP or placebo (three
tablets) was given at the time of enrolment into the trial and at all subsequent visits to
the antenatal clinic up to a maximum of four treatments. All women were given iron and folic
acid supplements as recommended by the Ministry of Health guidelines.
Surveillance
Women were visited at home twice per week by a project field worker to assess their health
and to encourage them to attend the ante-natal clinic at monthly intervals. Women with a
high risk of obstetric complications were encouraged to deliver in hospital but most women
delivered at home.
If a delivery occurred in hospital or a health center a finger prick blood sample was
obtained and the birth weight was measured. In the case of women who delivered at home, the
weight of the new born baby was measured within 5 days of delivery and a finger prick blood
sample obtained for measurement of Hb concentration and preparation of blood films.
Women were visited at home six weeks after delivery when an additional blood sample was
obtained and one year later to investigate the health of their child.
Laboratory methods
Hemoglobin concentration was measured using a Hemocue (Hemocue AB, Angelholm, Sweden). Thick
blood films were stained with Giemsa and examined for malaria parasites. Each slide was read
by two microscopists. If discrepant results were obtained, the slide was read by a third
microscopist and the majority view accepted.
Trial end-points
The co-primary trial end-points were hemoglobin concentration at, or shortly after, birth
and birthweight or weight of the baby shortly after birth.
Sample size
To detect a 20% reduction in the estimated risk of severe anemia (Hb <7 g/dl) among
multigravidae, estimated to be 30% in the control group, with 80 % power at the 5% level of
significance and allowing for a 30% loss to follow-up it was calculated that a study with
1115 women in each arm was required. To show a reduction in the proportion of low
birthweight babies from the expected 18% in the control group to 12% in the SP group with
80% power it was estimated that 2 x 1538 women would be needed. Thus, the target sample size
was 3,000.
Data management and analysis
All data were double entered and verified. Prior to the breaking of the code the data base
was locked and a copy given to the chair of the Data Safety Monitoring Board (DSMB).
Statistical analysis was done using S-plus and STATA. An analytical plan was prepared and
approved by the DSMB before the code was broken.
Trial oversight
The trial was monitored by a DSMB. It was conducted in line with the requirements of Good
Clinical Practice.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Double-Blind, Primary Purpose: Prevention
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