Malaria Clinical Trial
Official title:
A Double-blind, Randomised, Placebo-controlled Trial to Measure the Potential of Intermittent Treatment With Artesunate Plus Sulphadoxine/Pyrimethamine (SP) to Reduce the Malaria Burden in Sub-Saharan Africa
In countries of the Sahel and sub-Sahel, malaria transmission is highly seasonal with nearly
all infections occurring during a few months of the year. However, mortality and morbidity
from malaria may be high during this period, especially in young children who are the group
most at risk.
Intermittent preventative treatment (IPT) is a new approach to the prevention of malaria in
this situation. IPT involves the administration of an anti-malarial to children at risk for
malaria at fixed times, even if they are not infected. To investigate how effective this
approach might be in Senegal, a trial has been undertaken in which 1136 children aged 6
weeks to 59 months were given a single dose of sulfadoxine pyrimethamine and artesunate on
three occasions during a three-month rainy season and the incidence of clinical malaria in
these children was compared with that in a group of children who received placebo.
Additional observations were made on the incidence of side effects in children in the two
groups and on the impact of IPT in children (IPTc) on markers of drug resistance in children
whose blood films were positive for Plasmodium falciparum.
Background:
In countries of the Sahel and sub-Sahel, malaria transmission is highly seasonal.
Nevertheless, mortality and morbidity from malaria may be very high during the few months of
the year when malaria transmission takes place, especially in children. It has been shown
previously in The Gambia and elsewhere that in areas of seasonal malaria transmission,
mortality and morbidity from malaria in children can be reduced substantially by the regular
administration of anti-malarial drugs during the period of risk (chemoprophylaxis). However,
chemoprophylaxis is difficult to sustain. Intermittent preventative treatment (IPT) is an
adapted form of chemoprophylaxis in which anti-malarial drugs are given at fixed but less
frequent intervals than with chemoprophylaxis, allowing blood concentrations of
anti-malarial drugs to fall below the inhibitory concentration for periods between drug
administrations. This approach to malaria control was used first in pregnant women among
whom it is highly effective. However, more recently, it has also been used in infants (IPTi)
with anti-malarials being given at the same time as vaccines are administered. This approach
is likely to be most effective in areas of high transmission where a high proportion of
severe cases of malaria occur in children during the first year of life. IPTi is likely to
be less effective in reducing the burden of malaria in areas of seasonal malaria
transmission where many cases of severe malaria occur in older children. Intermittent
preventative treatment in children (IPTc) is a possible approach to the control of malaria
in areas where the main burden of malaria is in older children. Thus, the investigators have
undertaken a study to determine how effective this approach would be in preventing malaria
in Senegal.
Objectives:
The primary objective of the study was to determine whether the administration of one dose
of sulfadoxine-pyrimethamine plus artesunate to Senegalese children aged 6 weeks to 59
months on three occasions during the malaria transmission season would reduce significantly
the incidence of clinical attacks of malaria. Secondary objectives were determination of the
incidence of side effects in children who received IPTc; the impact of IPTc on the
prevalence of molecular markers of resistance to SP in samples positive for Plasmodium
falciparum; and the effects of IPTc on the incidence of malaria in the rainy season
following the intervention.
Study Area:
The study was conducted in Niakhar, a rural area in the centre of Senegal where malaria
transmission is very seasonal, nearly all transmission taking place during a three to four
month period. The entomological inoculation rate in the area is about 10 infectious bites
per person per year.
Study Population:
All children aged 6 weeks to 59 months residing in the study area were eligible to join the
study. There were few exclusion criteria (see below).
Study Procedure:
A series of meetings were held with members of the communities where the trial was
undertaken to explain its purpose. The families of potentially eligible children were
visited and asked if they wished their child to join the trial. If this was the case,
informed consent was obtained. Children were then allocated to one of eight randomisation
groups (four active drugs and four placebo).
At the start of the malaria transmission season, all study children were examined and a
finger-prick blood sample obtained for determination of packed cell volume and for
preparation of a thick blood film for microscopy. A drop of blood was collected onto filter
paper and stored for subsequent molecular studies. Children who were anaemic were treated. A
similar survey was conducted at the end of the malaria transmission season.
Following initial evaluation children were treated with either a single dose of
sulfadoxine-pyrimethamine and artesunate or with matching placebos. Treatment was repeated
on two further occasions separated by a period of a month. After each round of drug
administration a randomly selected group of children were visited and their parents or
guardians asked about any side effects related to the drug administration.
Surveillance for clinical attacks of malaria was undertaken through the detection of study
children when they presented to one of the clinics in the study area for treatment of a
febrile illness and through weekly home visits.
In the year following the treatment trial, children who had been randomised previously to
receive active drug or placebo were followed for another rainy season and the occurrence of
clinical attacks malaria detected as described above.
Blood films were stained with Giemsa and examined for malaria parasites by two experienced
microscopists. Parasite DNA was extracted from filter paper samples of children who were
parasitaemic and examined for mutations in the dhfr and dhps genes associated with
resistance to pyrimethamine and to sulphonamides respectively.
Trial End-Points:
The primary trial end-point was the incidence of clinical attacks of malaria in children who
received IPTc or placebo. Clinical malaria was defined as an episode of fever (temperature
recorded to be 37.5 degrees Celsius or higher or a history of fever within the previous 24
hours) for which no other cause could be found and the presences of P. falciparum
parasitaemia at a density of 3,000 parasites per microlitre or greater. This parasite
density was chosen as it has been shown previously to be an appropriate fever threshold in
the study area. Secondary end-points included the incidence of side effects in children in
each group, changes in the prevalences of resistance markers and the incidence of clinical
malaria in the year following the main trial.
Sample Size:
It was assumed on the basis of previous information that children in the control group would
experience an average of 0.4 clinical attacks of malaria during the malaria transmission
season. On the basis of this assumption, a trial with 540 children in each arm would have
80% power at the 5% level of significance to detect a 30% reduction in the incidence of
clinical attacks of malaria and a 90% power to detect a 40% reduction including an allowance
for a 10% drop-out during the surveillance period.
Monitoring:
The trial was monitored by an independent Data, Safety and Monitoring Board which reviewed
the study protocol, the standard operating procedures and the analytical plan.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Double-Blind, Primary Purpose: Prevention
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