Malaria Clinical Trial
Official title:
Neonatal Immune Dysfunction Associated to the Risk of Newborn Sepsis in Benin
The aim of the project is to study neonatal immune dysfunction associated to the risk of newborn sepsis in a malaria endemic area in Benin.
The fetal immunological responses maturate gradually during the last 3 months of pregnancy.
To respond to pathogens, newborns depend essentially on their innate immune system. Premature
babies have a significant impairment of innate and immune regulatory functions, thus
promoting neonatal sepsis. In addition, chronic infections during pregnancy, including those
of parasitic origin, fetal immunity. In utero exposure to P. falciparum antigens impacts
particularly the newborn immune development and is a risk factor predisposing to malaria and
also to other infections during the first year of life.
The major objectives are to assess:
- The relevance of a host biomarker driven diagnostic of sepsis in newborns,
- The relevance of immune markers as indicators of sepsis incidence, secondary infections
occurrence, and mortality
- The role of novel diagnostic techniques (FilmArray panels) as part of the
microbiological diagnostic,
- The immunological profile of the infants in the 3 first months of life.
The targeted population is newborns with a high risk to develop sepsis recruited at delivery
compared to a control infant population with a low infection risk.
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