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Diffusion MRI abnormalities after prolonged febrile seizures with encephalopathy

Authors :
Yoshihiro Maegaki
A. J. Barkovich
S. Fujimoto
Jun-ichi Takanashi
Mitsuhiro Kato
Masao Kawatani
Hiroko Tada
Hiroshi Ozawa
Tohru Okanishi
Y. Koyasu
Akira Sudo
Yuzo Tanabe
H. Oba
Hideo Yamanouchi
M. Ishitobi
Source :
Neurology. 66:1304-1309
Publication Year :
2006
Publisher :
Ovid Technologies (Wolters Kluwer Health), 2006.

Abstract

Background: Patients with encephalopathy heralded by a prolonged seizure as the initial symptom often have abnormal subcortical white matter on diffusion-weighted MRI (DWI). Objective: To determine if these patients share other common features. Methods: Patients with encephalopathy heralded by a prolonged seizure and followed by the identification of abnormal subcortical white matter on MRI were collected retrospectively. Their clinical, laboratory, and radiologic data were reviewed. Results: Seventeen patients were identified, ages 10 months to 4 years. All had a prolonged febrile seizure (longer than 1 hour in 12 patients) as their initial symptom. Subsequent seizures, most often in clusters of complex partial seizures, were seen 4 to 6 days after the initial seizure in 16 patients. Outcome ranged from almost normal to severe mental retardation. MRI performed within 2 days of presentation showed no abnormality. Subcortical white matter lesions were observed on DWI between 3 and 9 days in all 17 patients. T2-weighted images showed linear high intensity of subcortical U fibers in 13 patients. The lesions were predominantly frontal or frontoparietal in location with sparing of the perirolandic region. The diffusion abnormality disappeared between days 9 and 25, and cerebral atrophy was detected later than 2 weeks. Three patients having only frontal lesions had relatively good clinical outcome. Conclusions: Although the pathophysiologic mechanism remains unknown, these patients seem to have a distinctive encephalopathy syndrome. MRI is helpful in establishing the diagnosis of this encephalopathy.

Details

ISSN :
1526632X and 00283878
Volume :
66
Database :
OpenAIRE
Journal :
Neurology
Accession number :
edsair.doi.dedup.....710f9b876742d6acf57f40a614fb9d9e
Full Text :
https://doi.org/10.1212/01.wnl.0000210487.36667.a5