Abstract

BackgroundCongenital malaria is defined as malaria parasitaemia in the first week of life. The reported prevalence of congenital malaria in sub-Saharan Africa is variable (0 - 46%). Even though the clinical significance of congenital malaria parasitaemia is uncertain, anti-malarial drugs are empirically prescribed for sick newborns by frontline health care workers. Data on prevalence of congenital malaria in high-risk newborns will inform appropriate drug use and timely referral of sick newborns.MethodsBlood samples of untreated newborns less than 1 week of age at the time of referral to Korle Bu Teaching hospital in Accra, Ghana during the peak malaria seasons (April to July) of 2008 and 2010 were examined for malaria parasites by, i) Giemsa-stained thick and thin blood smears for parasite count and species identification, ii) histidine-rich protein- and lactic dehydrogenase-based rapid diagnosis tests, or iii) polymerase chain reaction amplification of the merozoite surface protein 2 gene, for identification of sub-microscopic parasitaemia. Other investigations were also done as clinically indicated.ResultsIn 2008, nine cases of Plasmodium falciparum parasitaemia were diagnosed by microscopy in 405 (2.2%) newborns. All the nine newborns had low parasite densities (≤50 per microlitre). In 2010, there was no case of parasitaemia by either microscopy or rapid diagnosis tests in 522 newborns; however, 56/467 (12%) cases of P. falciparum were detected by polymerase chain reaction.ConclusionCongenital malaria is an uncommon cause of clinical illness in high-risk untreated newborns referred to a tertiary hospital in the first week of life. Empirical anti-malarial drug treatment for sick newborns without laboratory confirmation of parasitaemia is imprudent. Early referral of sick newborns to hospitals with resources and skills for appropriate care is recommended.

Highlights

  • Congenital malaria is defined as malaria parasitaemia in the first week of life

  • This study presents the prevalence of malaria parasitaemia in non-treated high-risk newborns referred to a teaching hospital in the first week of life

  • Nine (2.2%) of the 405 newborns tested in 2008 had P. falciparum parasitaemia by microscopy, all of which were of low parasite density (≤50 per μl)

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Summary

Introduction

Congenital malaria is defined as malaria parasitaemia in the first week of life. Its effect as a cause of clinical disease in the newborn especially in the first week of life, when most newborn illnesses and deaths occur, is uncertain. Congenital malaria, defined as malaria parasitaemia in the first week of life can be acquired transplacentally or during the time of birth. Clinical malaria is rare in newborns from endemic areas with high incidence of malaria in pregnancy. This rare occurrence has been attributed to the transplacental transfer of maternally derived antibodies to malaria, and the inhibitory effect of foetal haemoglobin on malaria parasite development [10,11,12]

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