4.2 Article

Early clinical features and diagnosis of Dravet syndrome in 138 Chinese patients with SCN1A mutations

Journal

BRAIN & DEVELOPMENT
Volume 36, Issue 8, Pages 676-681

Publisher

ELSEVIER
DOI: 10.1016/j.braindev.2013.10.004

Keywords

Dxavet syndrome; SCN1A gene; Mutation; Febrile seizures; Diagnosis

Funding

  1. National Natural Science Foundation of China [81171221]

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Objective: To summarize the early clinical features of Dravet syndrome (DS) patients with SCN1A gene mutations before the age of one. Methods: SCN1A gene mutation screening was performed by PCR DNA sequencing and multiple ligation-dependent probe amplication (MLPA). The early clinical features of DS patients with SCN1A mutations were reviewed with attention to the seizures induced by fever and other precipitating factors before the first year of life. Results: The clinical data of 138 DS patients with SCN1A gene mutations were reviewed. The median seizure onset age was 5.3 months. Ninety-nine patients (71.7%) experienced seizures with duration more than 15 min in the first year of life. Two or more seizures induced by fever within 24 h or the same febrile illness were observed in 93 patients (67.4%). 111 patients (80.4%) had hemi-clonic and (or) focal seizures. Seizures had been triggered by fever of low degree (T< 38 degrees C) in 62.3% (86/138) before the first year of life. Vaccine-related seizures were observed in 34.8% (48/ 138). Seizures in 22.5% (31/138) of patients were triggered by hot bath. Carbamazepine, oxcarbazepine, lamotrigine, phenobarbital and phenytoin showed either no effect or exacerbating the seizures in our group. Conclusion: The seizure onset age in DS patients was earlier than that was in common febrile seizures. When a baby exhibits two or more features of complex febrile seizures in the first year of life, a diagnosis of DS should be considered, and SCN1A gene mutation screening should be performed as early as possible. Early diagnosis of DS will help clinicians more effectively prescribe antiepileptic drugs for stronger prognosis. (C) 2013 The Japanese Society of Child Neurology. Published by Elsevier B.V. All rights reserved.

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