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首页> 外文期刊>European journal of human genetics: EJHG >Detection of copy-number variation in AUTS2 gene by targeted exonic array CGH in patients with developmental delay and autistic spectrum disorders
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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

机译:靶向性外显子阵列CGH检测发育迟缓和自闭症谱系障碍患者AUTS2基因的拷贝数变异

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摘要

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. ? 2013 Macmillan Publishers Limited All rights reserved.
机译:最近,涉及单个基因的小基因组重排和拷贝数变异(CNV)与许多神经认知表型有关,包括智力残疾(ID),行为异常和自闭症谱系障碍(ASD)。自闭症易感性候选基因2(AUTS2)基因中的此类小CNV已显示与癫痫发作,ID和ASD相关。我们报告了四名患者的小型CNV,大小在133-319 kb之间,破坏了AUTS2。两名患者的重复涉及单个外显子,而两名患者的删除则去除了多个外显子。所有患者都有发育迟缓,而两名患者诊断为ASD。 CNV由外显子靶向阵列CGH检测,该外显子在已知或假设为多种人类表型的致病基因的外显子中具有密集的寡核苷酸覆盖。我们的报告进一步表明,破坏AUTS2会导致多种神经行为表型。更重要的是,它证明了靶向外显子阵列作为检测人类基因组临床相关区域中小的基因组重排的高度敏感的临床诊断工具的实用性。 ? 2013 Macmillan Publishers Limited保留所有权利。

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