CDKL5 mutations cause infantile spasms, early onset seizures, and severe mental retardation in female patients
- PMID: 16611748
- PMCID: PMC2564572
- DOI: 10.1136/jmg.2006.041467
CDKL5 mutations cause infantile spasms, early onset seizures, and severe mental retardation in female patients
Abstract
Objective: To determine the frequency of mutations in CDKL5 in both male and female patients with infantile spasms or early onset epilepsy of unknown cause, and to consider whether the breadth of the reported phenotype would be extended by studying a different patient group.
Methods: Two groups of patients were investigated for CDKL5 mutations. Group 1 comprised 73 patients (57 female, 16 male) referred to Cardiff for CDKL5 analysis, of whom 49 (42 female, 7 male) had epileptic seizure onset in the first six months of life. Group 2 comprised 26 patients (11 female, 15 male) with infantile spasms previously recruited to a clinical trial, the UK Infantile Spasms Study. Where a likely pathogenic mutation was identified, further clinical data were reviewed.
Results: Seven likely pathogenic mutations were found among female patients from group 1 with epileptic seizure onset in the first six months of life, accounting for seven of the 42 in this group (17%). No mutations other than the already published mutation were found in female patients from group 2, or in any male patient from either study group. All patients with mutations had early signs of developmental delay and most had made little developmental progress. Further clinical information was available for six patients: autistic features and tactile hypersensitivity were common but only one had suggestive Rett-like features. All had a severe epileptic seizure disorder, all but one of whom had myoclonic jerks. The EEG showed focal or generalised changes and in those with infantile spasms, hypsarrhythmia. Slow frequencies were seen frequently with a frontal or fronto-temporal predominance and high amplitudes.
Conclusions: The spectrum of the epileptic seizure disorder, and associated EEG changes, in those with CDKL5 mutations is broader than previously reported. CDKL5 mutations are a significant cause of infantile spasms and early epileptic seizures in female patients, and of a later intractable seizure disorder, irrespective of whether they have suspected Rett syndrome. Analysis should be considered in these patients in the clinical setting.
Conflict of interest statement
Conflicts of interest: none declared.
References
-
- Lux A L, Osborne J P. A proposal for case definitions and outcome measures in studies of infantile spasms and West syndrome: consensus statement of the West Delphi group. Epilepsia 2004451416–1428. - PubMed
-
- Manson J I. Tuberose sclerosis in childhood. Proc Aust Assoc Neurol 1973957–61. - PubMed
-
- Palmini A, Andermann F, Aicardi J, Dulac O, Chaves F, Ponsot G, Pinard J M, Goutieres F, Livingston J, Tampieri D. Diffuse cortical dysplasia, or the “double cortex” syndrome: the clinical and epileptic spectrum in 10 patients. Neurology 1991411656–1662. - PubMed
-
- Bingham P M, Spinner N B, Sovinsky L, Zackai E H, Chance P F. Infantile spasms associated with proximal duplication of chromosome 15q. Pediatr Neurol 199615163–165. - PubMed
-
- Gerard‐Blanluet M, Romana S, Munier C, Le Lorc'h M, Kanafani S, Sinico M, Touboul C, Levaillant J M, Haddad B, Lopez N, Lelong F, De Villemeur T B, Verloes A, Borghi E. Classical West “syndrome” phenotype with a subtelomeric 4p trisomy. Am J Med Genet 2004130A299–302. - PubMed
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