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From the Department of Pediatrics (G.M.R.), Faculty of Health Sciences, McMaster University, Hamilton, Ontario; Department of Pediatrics (D.B.), Faculty of Medicine, Memorial University of Newfoundland, St. John’s; The Janeway Child Health Centre (D.B., S.P.), St. John’s, Newfoundland; and Baycrest Centre & Department of Psychiatry (D.L.S.), University of Toronto, Ontario, Canada.
Address correspondence and reprint requests to Dr. Gabriel M. Ronen, HSC 3N11, 1200 Main Street West, Hamilton, Ontario, Canada L8N3Z5 roneng{at}mcmaster.ca
Objective: To examine outcome and explore for prognostic markers in a cohort <10 years following neonatal seizures.
Methods: We prospectively diagnosed clinical neonatal seizures with high specificity for true epileptic seizures in a population-based setting of all live newborns in the province of Newfoundland, Canada, between 1990 and 1995. Children with neonatal seizures were followed by specialized provincial health services. Follow-up data were collected on epilepsy, physical and cognitive impairments, and other heath issues.
Results: Data were available on 82 out of 90 subjects. We added information on six others whose outcome was clearly predictable from earlier information. Prognosis was better for term than for preterm infants (p = 0.003): term: 28 (45%) normal, 10 (16%) deaths, and 24 (39%) with impairments; preterm: 3 (12%) normal, 11 (42%) deaths, and 12 (46%) with impairments. Of survivors, 17 (27%) developed epilepsy, 16 (25%) had cerebral palsy, 13 (20%) had mental retardation, and 17 (27%) had learning disorders. Variables associated with poor prognosis were Sarnat stage III or equivalent severe encephalopathy, cerebral dysgenesis, complicated intraventricular hemorrhage, infections in the preterm infants, abnormal neonatal EEGs, and the need for multiple drugs to treat the neonatal seizures. Pure clonic seizures without facial involvement in term infants suggested favorable outcome, whereas generalized myoclonic seizures in preterm infants were associated with mortality.
Conclusions: Poor prognosis for premature infants with seizures is reflected in high rates of subsequent long-term disability and mortality. The severity and timing of the pathologic process continue to be the major determinants for outcome.
GLOSSARY: AED = antiepileptic drug; BW = birth weight; CLNESZ = clinical neonatal seizures; CP = cerebral palsy; GA = gestational age; IVH = intraventricular hemorrhage; LD = learning disability; MR = mental retardation; NCPP = National Collaborative Perinatal Project; NICU = neonatal intensive care unit.
Editorial, see page 1812
Supported by the Janeway Foundation.
Disclosure: The authors report no conflicts of interest.
Received December 11, 2006. Accepted in final form March 1, 2007.
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