Malaria Clinical Trial
Official title:
A Longitudinal Study Assessing the Infectious Status and Immunity of Mothers and Their Children in Lambaréné, Including Intermittent Treatment of Children With Sulfadoxine-pyrimethamine for Malaria Control and Its Impact on Long-term Health
The general goal of the project is to assess the infectious status and immunity of mothers and children living in a malaria region. A major part of the study involves administering an effective antimalarial, sulfadoxine-pyrimethamine (Fansidar®), to children at the same timepoints as vaccinations, i.e. at age 3, 9 and 15 months. The main objective is to study safety, efficacy, and consequences of such a strategy in particular the ability to reduce the risk of anemia.
More than 1.5 million deaths of African children under 5 years of age are due to Plasmodium
falciparum malaria. There is an urgent need for available and affordable strategies to
control malaria morbidity in childhood.
Malaria control measures have been assessed for their potential to reduce intensity of
infection in order to decrease the risk of malaria. It has been shown that malaria
prevention using drugs is potentially capable to reduce malaria morbidity, school
absenteeism, and all-cause mortality. However, prevention using drugs in the first years of
life can also result in the loss or delay of acquired resistance which can lead to a rebound
phenomenon (i.e. an increased risk of severe malaria after the therapy ended). In a recent
study on intermittent treatment with Fansidar® at 2, 3, and 9 months of age, the number of
malaria cases during the first 12 months of life was significantly reduced and no rebound
effect was observed. This study has demonstrated that the intermittent administration of
Fansidar® is safe and has beneficial effects for the children. However, the effectiveness
decreased some months after discontinuing the drug. The promising effect of the intermittent
administration of fansidar shown in this study needs to be confirmed in areas of different
endemicity such as Lambaréné, Gabon. It is assumed that a more extended intermittent
application of Fansidar® than performed in the above example would likely result in a longer
period of protection from malaria, and the extended intermittent administration of Fansidar
should not lead to rebound effects resulting in a higher occurrence of malaria.
The framework of this study offers a unique opportunity to study characteristics of
infectious disease of importance in the Lambaréné area and the development of resistance
against microbes at the maternofetal (mother/foetus) interface. Comparable studies will
simultaneously take place in two associated study sites (Kumasi and Tamale) with different
malaria endemicity in Ghana, West Africa.
Comparison: Comparison of malaria attacks in children with and without intermittent
Fansidar® treatment with drug administration at months 3 and 9 (alongside with routine
vaccinations delivered through child vaccination programme) and an additional administration
at month 15.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Prevention
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