Identification of Plasmodium falciparum and host factors associated with cerebral malaria: description of the protocol for a prospective, case-control study in Benin (NeuroCM)
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Abstract
Introduction Neonatal sepsis outreaches all causes of
neonatal mortality worldwide and remains a major societal
burden in low and middle income countries. In addition to
limited resources, endemic morbidities, such as malaria
and prematurity, predispose neonates and infants to
invasive infection by altering neonatal immune response
to pathogens. Nevertheless, thoughtful epidemiological,
diagnostic and immunological evaluation of neonatal
sepsis and the impact of gestational malaria have never
been performed.
Methods and analysis A prospective longitudinal
multicentre follow-up
of 580 infants from birth to 3 months
of age in urban and suburban Benin will be performed.
At delivery, and every other week, all children will be
examined and clinically evaluated for occurrence of sepsis.
At delivery, cord blood systematic analysis of selected
plasma and transcriptomic biomarkers (procalcitonin,
interleukin (IL)-6, IL-10, IP10, CD74 and CX3CR1)
associated with sepsis pathophysiology will be evaluated
in all live births as well as during the follow-up,
and when
sepsis will be suspected. In addition, whole blood response
to selected innate stimuli and extensive peripheral blood
mononuclear cells phenotypic characterisation will be
performed. Reference intervals specific to sub-Saharan
neonates will be determined from this cohort and
biomarkers performances for neonatal sepsis diagnosis
and prognosis tested.
Ethics and dissemination Ethical approval has been
obtained from the Comité d’Ethique de la Recherche –
Institut des Sciences Biomédicales Appliquées (CER-ISBA
85 - 5 April 2016, extended on 3 February 2017). Results
will be disseminated through international presentations
at scientific meetings and publications in peer-reviewed
journals.
