2013
DOI: 10.1002/aur.1284
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The Interstitial Duplication 15q11.2‐q13 Syndrome Includes Autism, Mild Facial Anomalies and a Characteristic EEG Signature

Abstract: Chromosomal copy number variants (CNV) are the most common genetic lesion found in autism. Many autism-associated CNVs are duplications of chromosome 15q. Although most cases of interstitial (int) dup(15) that present clinically are de novo and maternally derived or inherited, both pathogenic and unaffected paternal duplications of 15q have been identified. We performed a phenotype/genotype analysis of individuals with interstitial 15q duplications to broaden our understanding of the 15q syndrome and investiga… Show more

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Cited by 144 publications
(195 citation statements)
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“…Despite the well-known association between excess UBE3A and autism risk (4,5,53), including autism-linked mutations that elevate UBE3A alone (6,7), and extensive research on UBE3A (10), it is currently unclear how excess UBE3A affects mechanisms linked to autism and neurodevelopment. UBE3A is thought to be a promiscuous enzyme (54), and this seeming promiscuity has confounded attempts to identify the physiological substrates of UBE3A.…”
Section: Discussionmentioning
confidence: 99%
“…Despite the well-known association between excess UBE3A and autism risk (4,5,53), including autism-linked mutations that elevate UBE3A alone (6,7), and extensive research on UBE3A (10), it is currently unclear how excess UBE3A affects mechanisms linked to autism and neurodevelopment. UBE3A is thought to be a promiscuous enzyme (54), and this seeming promiscuity has confounded attempts to identify the physiological substrates of UBE3A.…”
Section: Discussionmentioning
confidence: 99%
“…This milder clinical phenotype in int dup (15) has been reported in previous studies. 13,35 Those with idic(15) had more severe epilepsy phenotypes, with mean EChess scores more than twice as high as those with int dup(15) (11.3 vs. 5.3). The rate of seizures in those with idic(15) (63%) was higher than reported previously in smaller cohorts, 5,8,30,31 but this may reflect response bias for families of individuals with seizures.…”
Section: Discussionmentioning
confidence: 99%
“…Parent-of-origin gene dosing appears to influence phenotype in idic (15); maternally inherited or derived interstitial duplications are associated with increased autism risk. 1,[10][11][12][13] Idic(15) chromosomes that include the BP2-BP3 region are virtually all maternally derived. Large maternally derived partial hexosomy for 15q11.2-q13 in two boys with intractable epilepsy further suggests that increased dosage of maternally expressed genes negatively impacts the idic(15) phenotype.…”
mentioning
confidence: 99%
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“…For instance, duplications on chromosome 15q11-q13 ('Dup15q syndrome') confer a very high risk for global developmental delay, hypotonia, ASD, ADHD, and epilepsy [49][50][51]. Quite notably, a subgroup of children with Dup15q syndrome exhibit a classic EEG pattern of excessive beta (12-30 Hz) frequency activity, a feature often found in patients treated with GABAergic medications such as benzodiazepenes [52].…”
Section: Diagnostic Biomarkers In Autism Spectrum Disordermentioning
confidence: 99%