Malaria Clinical Trial
Official title:
A Study Of Impact Of Intermittent Preventive Treatment In Children With Amodiaquine Plus Artesunate Versus Sulphadoxine-Pyrimethamine On Hemoglobin Levels And Malaria Morbidity In Hohoe District Of Ghana
Intermittent preventive treatment for malaria in children (IPTc) is a promising new approach to malaria control. Preliminary studies of IPTc in Senegal and Mali indicate that this approach can be very effective. Although the results of these studies suggest that IPTc with sulphadoxine-pyrimethamine (SP) plus artesunate (AS) or SP alone is an efficacious and safe intervention for reducing the burden of malaria and anaemia in children in high transmission areas with short transmission periods, there is no data from areas with long transmission periods. This study aims to evaluate the effectiveness of IPTc in reducing anaemia and malaria in an area with up to 6 months of transmission in Ghana. Two thousand two hundred forty children aged 3-59 months will be randomly allocated to four groups (560 per arm) to receive amodiaquine plus artesunate (AQ+AS), given at two different intervals (monthly or bimonthly), SP or placebo. The children will also be followed to determine if there is any rebound in the incidence of severe malaria and anaemia in the year following IPTc.
Background:
In high transmission areas, where a major proportion of deaths and severe morbidity from
malaria occurs during the first year of life, intermittent preventive treatment for infants
(IPTi) could make a major contribution to reducing the burden of malaria as a whole.
However, in many areas in Africa, where mortality and morbidity from malaria in children
under five years of age is very high and the burden of malaria is not predominantly in
infants, IPTi, even if highly effective, would have only a limited impact on the overall
burden of malaria in children.
Few community trials have evaluated the effect of IPTc in the prevention of malaria. Dicko
and his colleagues in Mali, an area of seasonal malaria transmission gave two doses of SP to
children aged 6 months to 9 years at an interval of two months and found a protective
efficacy of 40% against clinical attacks of malaria among children in the intervention group
compared to the placebo group. Recent work in Niakhar, Senegal has assessed IPTc in an area
of intense but short seasonal malaria transmission. The study used a combination of SP plus
one dose of AS, which was given every month for three months during the rainy season which
lasted for only four months. This study showed that IPTc using AS+SP was well tolerated
without any drug-attributable adverse events and that IPTc can reduce the incidence of
clinical malaria by 86%. Although these results suggest that IPTc with SP+one dose of AS is
an efficacious and safe intervention for reducing the burden of malaria and anaemia in
children, there is no data on the effectiveness of IPTc in areas with prolonged transmission
seasons and on the use of other forms of combination therapy in IPTc.
Study overview:
The study aims to determine the optimum drug schedule for IPTc in an area of prolonged
seasonal malaria transmission in Ghana. The main study will compare the effectiveness of
IPTC using SP, monthly AQ+AS or bimonthly AQ+AS. In order to facilitate the interpretation
of the results of this trial, two ancillary studies will be done. The first will be a
conventional in vivo drug efficacy study of SP and AQ+AS in children with clinical malaria
to ensure the efficacy of the drugs used in the IPTc trial within the study area. The second
subsidiary study will be an investigation of whether or not administration of IPTc over one
malaria transmission season is followed by an increase in the incidence of malaria or
anaemia during the following malaria transmission season.
Study Objectives:
1. To investigate whether IPTc using monthly or bimonthly AQ+AS or SP can improve mean Hb
level and decrease anaemia and malaria morbidity in young children in an area of
intense and prolonged seasonal malaria transmission.
2. To compare the incidence of severe malaria among children aged 3-59 months using the
three treatment regimens.
Study area:
The study will be carried out in Hohoe district, Ghana. The major rainy season lasts from
April to July and the minor one from September to November. The rest of the year is
relatively dry. Malaria is the most common disease in this area. For the past four years
malaria has accounted for 32% of the out patient attendances out of which 45% were children
under five years. Twenty five percent (25%) of malaria cases required inpatient care and 37%
of the cases were children under five years and 57% of them reported with anaemia. The peak
of OPD malaria and anaemia cases occurs between June and October.
Study procedures:
A cross-sectional survey will be carried out after informed consent has been obtained from
the guardians of all children aged between 3 to 59 months in the selected villages.
Information will be collected on the background of the child and guardian, hypersensitivity
to the study drugs and bednet use. Anthropometric indices will be measured.
Drugs will be administered to the study children every month from May to October. Field
workers and coordinators will visit the participants once a week from May to October.
Parents and guardians will be strongly advised to come directly to a health centre if their
child develops any symptoms or signs of illness between the field workers' weekly
home-visits. Passive surveillance will be performed by six medical assistants and twelve
nurses based in the health centres in the sub-districts within the district. Malaria
clinical attacks will be documented and treatment for malaria and any other illness will be
provided free of charge to study participants in all the health centres that are in the
catchment area of the selected communities.
If the child has fever or any features suggestive of malaria, a finger prick blood sample
will be collected for Hb and malaria parasite detection. Two slides will be prepared for
each child. At the health centre, one slide will be examined on the same day for deciding on
appropriate treatment. The second slide will be kept and sent to the central laboratory for
reading to provide a definitive diagnosis. Those who have malaria will be treated with oral
quinine 10mg/kg every 8 hours for 7days and will be followed on days 3 and 7 for outcome
measurement.
At the end of the malaria transmission season, a cross-sectional survey will be undertaken
involving all children who have remained in the study. Following administration of a short
questionnaire, a finger prick blood sample will be obtained for preparation of a blood film
and for determination of Hb. A filter paper sample will be collected for molecular studies.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Outcomes Assessor), Primary Purpose: Prevention
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