TY - JOUR
T1 - How should children with West syndrome be efficiently and accurately investigated? Results from the National Infantile Spasms Consortium
AU - Pediatric Epilepsy Research Consortium (PERC)
AU - Wirrell, Elaine C.
AU - Shellhaas, Renéee A.
AU - Joshi, Charuta
AU - Keator, Cynthia
AU - Kumar, Shilpi
AU - Mitchell, Wendy G.
AU - Berg, A.
AU - Brooks-Kayal, A.
AU - Coryell, J.
AU - Dlugos, D.
AU - Gaillard, W. D.
AU - Goodkin, H.
AU - Grinspan, Z.
AU - Jansen, L.
AU - Knupp, K.
AU - Kossoff, E.
AU - Hartman, A. L.
AU - Hussain, S.
AU - Joshi, S.
AU - Loddenkemper, T.
AU - Millichap, J. J.
AU - Mytinger, J.
AU - Nickels, K.
AU - Nordli, D.
AU - Ryan, N.
AU - Sanchez-Fernandez, I.
AU - Sullivan, J.
AU - Valencia, I.
AU - Wong-Kisiel, L.
AU - Wusthoff, C.
AU - Yozawitz, E.
N1 - Publisher Copyright:
© Wiley Periodicals, Inc. © 2015 International League Against Epilepsy.
PY - 2015/4/1
Y1 - 2015/4/1
N2 - Summary Objective To prospectively evaluate the etiology of new-onset infantile spasms and evaluate the yield of genetic and metabolic investigations in those without obvious cause after initial clinical evaluation and magnetic resonance imaging (MRI). Methods Twenty-one U.S. pediatric epilepsy centers prospectively enrolled infants with newly diagnosed West syndrome in a central database. Etiology and investigations performed within 3 months of diagnosis were documented. Results From June 2012 to June 2014, a total of 251 infants were enrolled (53% male). A cause was identified in 161 (64.4%) of 250 cases (genetic,14.4%; genetic-structural, 10.0%; structural-congenital, 10.8%; structural-acquired, 22.4%; metabolic, 4.8%; and infectious, 2.0%). An obvious cause was found after initial clinical assessment (history and physical examination) and/or MRI in 138 of 161, whereas further genetic and metabolic studies were revealing in another 23 cases. Of 112 subjects without an obvious cause after initial evaluation and MRI, 81 (72.3%) had undergone genetic testing, which showed a causal abnormality in 23.5% and a variant of unknown significance in 14.8%. Although metabolic studies were done in the majority (serum, 79.5%; urine, 69.6%; and cerebrospinal fluid [CSF], 38.4%), these revealed an etiology in only five cases (4.5%). No correlation was found between type of health insurance (public vs. private) and either genetic or metabolic testing. Significance Clinical evaluation and MRI provide a specific diagnosis in 55% of children presenting with West syndrome. We propose that a cost-effective workup for those without obvious cause after initial clinical evaluation and MRI includes an array comparative genomic hybridization (aCGH) followed by an epilepsy gene panel if the microarray is not definitive, serum lactate, serum amino acids, and urine organic acids.
AB - Summary Objective To prospectively evaluate the etiology of new-onset infantile spasms and evaluate the yield of genetic and metabolic investigations in those without obvious cause after initial clinical evaluation and magnetic resonance imaging (MRI). Methods Twenty-one U.S. pediatric epilepsy centers prospectively enrolled infants with newly diagnosed West syndrome in a central database. Etiology and investigations performed within 3 months of diagnosis were documented. Results From June 2012 to June 2014, a total of 251 infants were enrolled (53% male). A cause was identified in 161 (64.4%) of 250 cases (genetic,14.4%; genetic-structural, 10.0%; structural-congenital, 10.8%; structural-acquired, 22.4%; metabolic, 4.8%; and infectious, 2.0%). An obvious cause was found after initial clinical assessment (history and physical examination) and/or MRI in 138 of 161, whereas further genetic and metabolic studies were revealing in another 23 cases. Of 112 subjects without an obvious cause after initial evaluation and MRI, 81 (72.3%) had undergone genetic testing, which showed a causal abnormality in 23.5% and a variant of unknown significance in 14.8%. Although metabolic studies were done in the majority (serum, 79.5%; urine, 69.6%; and cerebrospinal fluid [CSF], 38.4%), these revealed an etiology in only five cases (4.5%). No correlation was found between type of health insurance (public vs. private) and either genetic or metabolic testing. Significance Clinical evaluation and MRI provide a specific diagnosis in 55% of children presenting with West syndrome. We propose that a cost-effective workup for those without obvious cause after initial clinical evaluation and MRI includes an array comparative genomic hybridization (aCGH) followed by an epilepsy gene panel if the microarray is not definitive, serum lactate, serum amino acids, and urine organic acids.
KW - Diagnostic test assessment
KW - Infantile spasms
KW - Observational cohort
KW - Pediatric
KW - West syndrome
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U2 - 10.1111/epi.12951
DO - 10.1111/epi.12951
M3 - Article
C2 - 25779538
AN - SCOPUS:84927510091
SN - 0013-9580
VL - 56
SP - 617
EP - 625
JO - Epilepsia
JF - Epilepsia
IS - 4
ER -