BMJ 1995;311:598-602 (2 September)

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Predictors of neonatal encephalopathy in full term infants

Stuart J Adamson, student,a Louisa M Alessandri, research officer,a Nadia Badawi, paediatric research fellow,a Paul R Burton, senior biostatistician,a Patrick J Pemberton, director,b Fiona Stanley, director a

a Institute for Child Health Research, PO Box 855, West Perth 6872, Western Australia, Australia, b Department of Neonatology, Princess Margaret Hospital for Children, Subiacco 6008 Western Australia

Correspondence to: Professor Stanley.

Abstract

Objective: Preliminary investigation of the contribution of adverse antepartum and intrapartum factors to neonatal encephalopathy in singleton neonates born full term.
Design: Matched case-control study based on incidence density sampling of controls.
Setting: Two major teaching hospitals (one paediatric and one obstetric) and three peripheral maternity hospitals in Perth, Western Australia (population 1.2 million).
Subjects: 89 cases, all the full term singleton neonates born during an eight month period in 1992 who fulfilled one or more of six criteria during the first week of life (seizures, abnormal conscious state, persistent hypertonia or hypotonia, and feeding or respiratory difficulties of central origin). One full term control infant without neonatal encephalopathy was matched to each case by sex, hospital of delivery, time of day and day of the week of birth, and maternal health insurance status.
Main outcome measures: Odds ratio estimates of relative risk of neonatal encephalopathy associated with antepartum and intrapartum factors.
Results: Estimated incidence of moderate or severe encephalopathy in first week of life was 3.75 per 1000 full term live births. Thirteen cases and no controls had evidence suggestive of important intrapartum hypoxia, and in only five of these cases was the neurological condition at birth attributed to events during the intrapartum period. Univariate conditional logistic regression analysis identified significant differences between cases and controls for maternal vaginal bleeding in pregnancy, maternal thyroxine treatment, congenital abnormalities, induction of labour, interval from membrane rupture to delivery, maternal pyrexia in labour, augmentation of labour, abnormal intrapartum cardiotocograms, and meconium in labour. Family history of convulsions also approached significance.
Conclusions: Our preliminary results suggest that intrapartum hypoxia, according to currently used criteria, was not the cause of neonatal encephalopathy in most cases in this population. Our findings suggest that many aetiologies of neonatal encephalopathy originate in the antepartum period.

Key messages

  • Key messages

  • In this study the incidence of moderate or severe encephalopathy was found to be 3.75 per 1000 live term births, with a case fatality of almost 8%

  • Intrapartum hypoxia, determined with tradi- tional criteria, was not the cause of neonatal encephalopathy in most cases

  • Signs of intrapartum fetal distress may be the first signs of pre-existing neurological abnor- mality, and events occurring in the antepartum period are an important cause of neurological abnormality in newborn infants

  • These results have implications for obste- tricians, paediatricians, and legal practitioners


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