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Detection of copy-number variation in AUTS2 gene by targeted exonic array CGH in patients with developmental delay and autistic spectrum disorders
Authors:Sandesh C S Nagamani  Ayelet Erez  Bruria Ben-Zeev  Moshe Frydman  Susan Winter  Robert Zeller  Dima El-Khechen  Luis Escobar  Pawel Stankiewicz  Ankita Patel  Sau Wai Cheung
Affiliation:1.Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, TX, USA;2.Pediatric Neurology Unit, Safra Children''s Hospital, Sheba Medical center, Tel Hashomer, Israel;3.Genetics Institute, Sheba Medical center, Tel Hashomer, Israel;4.Children''s Hospital Central California, Madera, CA, USA;5.Department of Pediatrics, Baylor College of Medicine, Houston, TX, USA;6.Peyton Manning Children''s Hospital, Indianapolis, IN, USA
Abstract:
Small genomic rearrangements and copy-number variations (CNVs) involving a single gene have been associated recently with many neurocognitive phenotypes, including intellectual disability (ID), behavioral abnormalities, and autistic spectrum disorders (ASDs). Such small CNVs in the Autism susceptibility candidate 2 (AUTS2) gene have been shown to be associated with seizures, ID, and ASDs. We report four patients with small CNVs ranging in size between 133–319 kb that disrupt AUTS2. Two patients have duplications involving single exons, whereas two have deletions that removed multiple exons. All patients had developmental delay, whereas two patients had a diagnosis of ASDs. The CNVs were detected by an exon-targeted array CGH with dense oligonucleotide coverage in exons of genes known or hypothesized to be causative of multiple human phenotypes. Our report further shows that disruption of AUTS2 results in a variety of neurobehavioral phenotypes. More importantly, it demonstrates the utility of targeted exon array as a highly sensitive clinical diagnostic tool for the detection of small genomic rearrangements in the clinically relevant regions of the human genome.
Keywords:intellectual disability   targeted exon array   AUTS2
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