Duplications of 17q12 can cause familial fever-related epilepsy syndromes

Objectives: After we identified a 17q12 duplication cosegregating in a 4-generation family with genetic or generalized epilepsy with febrile seizures plus (GEFS+), we aimed to determine the frequency of 17q12 genomic rearrangements in GEFS+ and a wide spectrum of other epilepsy phenotypes. We furthermore describe seizure prevalence in previously reported patients with a 17q12 duplication or deletion. Methods: We analyzed 433 patients with a broad range of epilepsy phenotypes. The 180k Cytosure ISCA v2 array was used for copy number variation screening in the index patient. Segregation analysis and follow-up studies were performed with the multiplex amplicon quantification technique. Results: We identified 2 families in which a 17q12 duplication segregated with febrile-sensitive epilepsy. In the follow-up study, the mutation rate in familial febrile seizures (FS) and GEFS+ phenotypes was 1/222. No 17q12 deletions were detected. Two of the 6 mutation carriers in the initial GEFS+ family had mild intellectual disability, whereas all family members of the second family were of normal intelligence. In the literature, 4 of 43 individuals with a 17q12 duplication and 4 of 55 with the reciprocal deletion were described to have had seizures. Conclusions: Our study shows that 17q12 duplications are a rare cause of familial FS and GEFS+. Although some family members might have intellectual disability, seizures can be the sole clinical symptom. This is the first report on an inherited copy number variation in these self-limiting fever-sensitive epilepsy syndromes, potentially revealing a novel pathomechanism involved in familial FS and GEFS+.

[1]  Peter J. Scambler,et al.  22q11.2 deletion syndrome. , 2015, Nature reviews. Disease primers.

[2]  Donna M. Martin,et al.  Phenotypic heterogeneity of genomic disorders and rare copy-number variants. , 2012, The New England journal of medicine.

[3]  S. Brucker,et al.  Frame shift mutation of LHX1 is associated with Mayer-Rokitansky-Kuster-Hauser (MRKH) syndrome. , 2012, Human reproduction.

[4]  R. Harrison,et al.  17q12 microdeletion syndrome: Three patients illustrating the phenotypic spectrum , 2012, American Journal of Medical Genetics. Part A.

[5]  J. Kearney Advances in Epilepsy Genetics and Genomics , 2012, Epilepsy currents.

[6]  J. Vermeesch,et al.  Genome‐wide arrays: Quality criteria and platforms to be used in routine diagnostics , 2012, Human mutation.

[7]  H. Bolz,et al.  A complex microdeletion 17q12 phenotype in a patient with recurrent de novo membranous nephropathy , 2012, BMC Nephrology.

[8]  A. Kolevzon,et al.  Complex autism spectrum disorder in a patient with a 17q12 microduplication , 2012, American journal of medical genetics. Part A.

[9]  M. Fichera,et al.  Clinical significance of rare copy number variations in epilepsy: a case-control survey using microarray-based comparative genomic hybridization. , 2012, Archives of neurology.

[10]  Zi-jiang Chen,et al.  LHX1 mutation screening in 96 patients with müllerian duct abnormalities. , 2012, Fertility and sterility.

[11]  D. Love,et al.  Recurrent Transmission of a 17q12 Microdeletion and a Variable Clinical Spectrum , 2011, Molecular Syndromology.

[12]  U. Surti,et al.  Prenatally Diagnosed 17q12 Microdeletion Syndrome with a Novel Association with Congenital Diaphragmatic Hernia , 2011, Fetal Diagnosis and Therapy.

[13]  I. Scheffer,et al.  Rare copy number variants are an important cause of epileptic encephalopathies , 2011, Annals of neurology.

[14]  J. Buizer-Voskamp,et al.  Genome Arrays for the Detection of Copy Number Variations in Idiopathic Mental Retardation, Idiopathic Generalized Epilepsy and Neuropsychiatric Disorders: Lessons for Diagnostic Workflow and Research , 2011, Cytogenetic and Genome Research.

[15]  Carlos S. Moreno,et al.  Relative Burden of Large CNVs on a Range of Neurodevelopmental Phenotypes , 2011, PLoS genetics.

[16]  P. Calvas,et al.  A 17q12 chromosomal duplication associated with renal disease and esophageal atresia. , 2011, European journal of medical genetics.

[17]  M. Beckmann,et al.  Recurrent aberrations identified by array-CGH in patients with Mayer-Rokitansky-Küster-Hauser syndrome. , 2011, Fertility and sterility.

[18]  Urvashi Surti,et al.  Deletion 17q12 is a recurrent copy number variant that confers high risk of autism and schizophrenia. , 2010, American journal of human genetics.

[19]  C. Bellanné-Chantelot,et al.  Autism in three patients with cystic or hyperechogenic kidneys and chromosome 17q12 deletion. , 2010, Nephrology, dialysis, transplantation : official publication of the European Dialysis and Transplant Association - European Renal Association.

[20]  B. Torchia,et al.  Deletion of hepatocyte nuclear factor-1-beta in an infant with prune belly syndrome. , 2010, American journal of perinatology.

[21]  Ulrich Stephani,et al.  Genome-Wide Copy Number Variation in Epilepsy: Novel Susceptibility Loci in Idiopathic Generalized and Focal Epilepsies , 2010, PLoS genetics.

[22]  P. Stankiewicz,et al.  Clinical spectrum associated with recurrent genomic rearrangements in chromosome 17q12 , 2010, European Journal of Human Genetics.

[23]  F. Speleman,et al.  Multiplex Amplicon Quantification (MAQ), a fast and efficient method for the simultaneous detection of copy number alterations in neuroblastoma , 2010, BMC Genomics.

[24]  S. Gimelli,et al.  Recurrent microdeletion at 17q12 as a cause of Mayer-Rokitansky-Kuster-Hauser (MRKH) syndrome: two case reports , 2009, Orphanet journal of rare diseases.

[25]  B. Plecko,et al.  Vitamin B6 dependent seizures. , 2009, The Canadian journal of neurological sciences. Le journal canadien des sciences neurologiques.

[26]  I. Scheffer,et al.  Dravet syndrome or genetic (generalized) epilepsy with febrile seizures plus? , 2009, Brain and Development.

[27]  A. Renieri,et al.  Private inherited microdeletion/microduplications: implications in clinical practice. , 2008, European Journal of Medical Genetics.

[28]  C. Kim,et al.  Genomic imbalances associated with müllerian aplasia , 2007, Journal of Medical Genetics.

[29]  H. Mefford,et al.  Recurrent reciprocal genomic rearrangements of 17q12 are associated with renal disease, diabetes, and epilepsy. , 2007, American journal of human genetics.

[30]  J. Lupski,et al.  Genomic Rearrangements and Gene Copy-Number Alterations as a Cause of Nervous System Disorders , 2006, Neuron.

[31]  A. McMahon,et al.  Distinct and sequential tissue-specific activities of the LIM-class homeobox gene Lim1 for tubular morphogenesis during kidney development , 2005, Development.

[32]  D. Fitzpatrick,et al.  MLYCD mutation analysis: Evidence for protein mistargeting as a cause of MLYCD deficiency , 2003, Human mutation.

[33]  I. Scheffer,et al.  Mutations in the human ortholog of Aristaless cause X-linked mental retardation and epilepsy , 2002, Nature Genetics.

[34]  I. Scheffer,et al.  Generalized epilepsy with febrile seizures plus. A genetic disorder with heterogeneous clinical phenotypes. , 1997, Brain : a journal of neurology.

[35]  P. Matthews,et al.  Pyruvate dehydrogenase deficiency: Molecular basis for intrafamilial heterogeneity , 1994, Annals of neurology.

[36]  K. Kim,et al.  Structure of the coding sequence and primary amino acid sequence of acetyl-coenzyme A carboxylase. , 1988, Proceedings of the National Academy of Sciences of the United States of America.