Abstract

Background: Bilirubin encephalopathy is the clinical syndrome associated with bilirubin toxicity to the central nervous system resulting in chronic and permanent sequelae. It has been estimated that approximately 60% of term babies and 80% of preterm babies develop jaundice within the first week of life. Objective: To determine the prevalence, morbidity and mortality of bilirubin encephalopathy at our centre. Methodology: A retrospective descriptive review of the case files of all babies diagnosed with bilirubin encephalopathy over the past 5 years from January 2010 to December 2014 was undertaken. Information retrieved from the case notes included age, sex, presence of fever, duration of illness, place of delivery, causes and treatment. The outcome measures such as discharged home, discharged against medical advice, and death were also noted. Results: Out of a total of 2,820 babies, 21 (0.74%) were admitted on account of bilirubin encephalopathy. Of these 21, seventeen (81%) were males and four (19%) females giving M; F ratio of 5:1. Eighteen babies (85.7%) had pyrexia, 8(38.1%) and 6(28.6%) were hypertonic and hypotonic respectively on admission. Only 33.3% of the deliveries took place in the health facilities. The established factors responsible for jaundice included infections (septicaemia) (15/71.4%), ABO incompatibility (4/19.1%), and G6PDeficiency (2/9.5%). The mean maximum serum bilirubin of the subjects was 321.3μmol/l (242.5 – 440.3). The case fatality was 4/21(19%). Conclusion: Neonatal septicaemia is associated with bilirubin encephalopathy. Therefore identification and prompt treatment is of utmost importance to avoid morbidity and mortality.

Highlights

  • Bilirubin is the breakdown product of haem, a content/component of the red blood cells

  • Neonatal septicaemia is associated with bilirubin encephalopathy

  • Identification and prompt treatment is of utmost importance to avoid morbidity and mortality

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Summary

Introduction

Bilirubin is the breakdown product of haem, a content/component of the red blood cells. A rise in blood levels of this pigment can cause jaundice, a yellow colouration of the skin and sclera. Neuronal damage/toxicity occurs as a result of increased concentration of unconjugated/free or unbound bilirubin in the blood. Unconjugated bilirubin crosses the blood brain barrier when the bilirubin binding capacity is exceeded. Bilirubin encephalopathy (BE) is the clinical syndrome associated with bilirubin toxicity to the central nervous system while Kenicterus is the pathological or anatomic diagnosis made at autopsy resulting in chronic and permanent sequel. It has been estimated that approximately 60% of term babies and 80% of preterm. Bilirubin encephalopathy is the clinical syndrome associated with bilirubin toxicity to the central nervous system resulting in chronic and permanent sequelae. It has been estimated that approximately 60% of term babies and 80% of preterm babies develop jaundice within the first week of life

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