TY - JOUR
T1 - Structural genomic variation in childhood epilepsies with complex phenotypes
AU - Helbig, Ingo
AU - Swinkels, Marielle E M
AU - Aten, Emmelien
AU - Caliebe, Almuth
AU - van 't Slot, Ruben
AU - Boor, Rainer
AU - von Spiczak, Sarah
AU - Muhle, Hiltrud
AU - Jähn, Johanna A
AU - van Binsbergen, Ellen
AU - van Nieuwenhuizen, Onno
AU - Jansen, Floor E
AU - Braun, Kees P J
AU - de Haan, Gerrit-Jan
AU - Tommerup, Niels
AU - Stephani, Ulrich
AU - Hjalgrim, Helle
AU - Poot, Martin
AU - Lindhout, Dick
AU - Brilstra, Eva H
AU - Møller, Rikke S
AU - Koeleman, Bobby P C
PY - 2014/7
Y1 - 2014/7
N2 - A genetic contribution to a broad range of epilepsies has been postulated, and particularly copy number variations (CNVs) have emerged as significant genetic risk factors. However, the role of CNVs in patients with epilepsies with complex phenotypes is not known. Therefore, we investigated the role of CNVs in patients with unclassified epilepsies and complex phenotypes. A total of 222 patients from three European countries, including patients with structural lesions on magnetic resonance imaging (MRI), dysmorphic features, and multiple congenital anomalies, were clinically evaluated and screened for CNVs. MRI findings including acquired or developmental lesions and patient characteristics were subdivided and analyzed in subgroups. MRI data were available for 88.3% of patients, of whom 41.6% had abnormal MRI findings. Eighty-eight rare CNVs were discovered in 71 out of 222 patients (31.9%). Segregation of all identified variants could be assessed in 42 patients, 11 of which were de novo. The frequency of all structural variants and de novo variants was not statistically different between patients with or without MRI abnormalities or MRI subcategories. Patients with dysmorphic features were more likely to carry a rare CNV. Genome-wide screening methods for rare CNVs may provide clues for the genetic etiology in patients with a broader range of epilepsies than previously anticipated, including in patients with various brain anomalies detectable by MRI. Performing genome-wide screens for rare CNVs can be a valuable contribution to the routine diagnostic workup in patients with a broad range of childhood epilepsies.
AB - A genetic contribution to a broad range of epilepsies has been postulated, and particularly copy number variations (CNVs) have emerged as significant genetic risk factors. However, the role of CNVs in patients with epilepsies with complex phenotypes is not known. Therefore, we investigated the role of CNVs in patients with unclassified epilepsies and complex phenotypes. A total of 222 patients from three European countries, including patients with structural lesions on magnetic resonance imaging (MRI), dysmorphic features, and multiple congenital anomalies, were clinically evaluated and screened for CNVs. MRI findings including acquired or developmental lesions and patient characteristics were subdivided and analyzed in subgroups. MRI data were available for 88.3% of patients, of whom 41.6% had abnormal MRI findings. Eighty-eight rare CNVs were discovered in 71 out of 222 patients (31.9%). Segregation of all identified variants could be assessed in 42 patients, 11 of which were de novo. The frequency of all structural variants and de novo variants was not statistically different between patients with or without MRI abnormalities or MRI subcategories. Patients with dysmorphic features were more likely to carry a rare CNV. Genome-wide screening methods for rare CNVs may provide clues for the genetic etiology in patients with a broader range of epilepsies than previously anticipated, including in patients with various brain anomalies detectable by MRI. Performing genome-wide screens for rare CNVs can be a valuable contribution to the routine diagnostic workup in patients with a broad range of childhood epilepsies.
U2 - 10.1038/ejhg.2013.262
DO - 10.1038/ejhg.2013.262
M3 - Journal article
C2 - 24281369
SN - 1018-4813
VL - 22
SP - 896
EP - 901
JO - European Journal of Human Genetics
JF - European Journal of Human Genetics
IS - 7
ER -