Seaver Autism Center for Research and Treatment, Department of Psychiatry, Mount Sinai School of Medicine, New York, NY 10029, USA.
Mol Autism. 2010 Mar 19;1(1):5. doi: 10.1186/2040-2392-1-5.
The 15q24 microdeletion syndrome has been recently described as a recurrent, submicroscopic genomic imbalance found in individuals with intellectual disability, typical facial appearance, hypotonia, and digital and genital abnormalities. Gene dosage abnormalities, including copy number variations (CNVs), have been identified in a significant fraction of individuals with autism spectrum disorders (ASDs). In this study we surveyed two ASD cohorts for 15q24 abnormalities to assess the frequency of genomic imbalances in this interval.
We screened 173 unrelated subjects with ASD from the Central Valley of Costa Rica and 1336 subjects with ASD from 785 independent families registered with the Autism Genetic Resource Exchange (AGRE) for CNVs across 15q24 using oligonucleotide arrays. Rearrangements were confirmed by array comparative genomic hybridization and quantitative PCR.
Among the patients from Costa Rica, an atypical de novo deletion of 3.06 Mb in 15q23-q24.1 was detected in a boy with autism sharing many features with the other 13 subjects with the 15q24 microdeletion syndrome described to date. He exhibited intellectual disability, constant smiling, characteristic facial features (high anterior hairline, broad medial eyebrows, epicanthal folds, hypertelorism, full lower lip and protuberant, posteriorly rotated ears), single palmar crease, toe syndactyly and congenital nystagmus. The deletion breakpoints are atypical and lie outside previously characterized low copy repeats (69,838-72,897 Mb). Genotyping data revealed that the deletion had occurred in the paternal chromosome. Among the AGRE families, no large 15q24 deletions were observed.
From the current and previous studies, deletions in the 15q24 region represent rare causes of ASDs with an estimated frequency of 0.1 to 0.2% in individuals ascertained for ASDs, although the proportion might be higher in sporadic cases. These rates compare with a frequency of about 0.3% in patients ascertained for unexplained intellectual disability and congenital anomalies. This atypical deletion reduces the minimal interval for the syndrome from 1.75 Mb to 766 kb, implicating a reduced number of genes (15 versus 38). Sequencing of genes in the 15q24 interval in large ASD and intellectual disability samples may identify mutations of etiologic importance in the development of these disorders.
15q24 微缺失综合征是一种新近发现的、重复出现的亚显微基因组不平衡,发生于伴有智力障碍、典型面部特征、肌张力低下、以及数字和生殖器异常的个体中。包括拷贝数变异(CNVs)在内的基因剂量异常,已经在很大一部分自闭症谱系障碍(ASD)个体中被识别。在这项研究中,我们对两个 ASD 队列进行了 15q24 异常的筛查,以评估该区间内基因组失衡的频率。
我们使用寡核苷酸微阵列对来自哥斯达黎加中央山谷的 173 名 ASD 无关个体和登记在自闭症基因资源交换(AGRE)中的 785 个独立家庭的 1336 名 ASD 个体进行了 15q24 上的 CNVs 筛查。通过比较基因组杂交和定量 PCR 对重排进行了确认。
在来自哥斯达黎加的患者中,我们检测到了一名患有自闭症的男孩的一个非典型的新发 3.06 Mb 的 15q23-q24.1 缺失,该男孩与迄今报道的其他 13 名患有 15q24 微缺失综合征的患者具有许多共同特征。他表现出智力障碍、持续微笑、典型的面部特征(高发际线、宽的内眉、内眦赘皮、远视、饱满的下唇和突出、后旋的耳朵)、单一掌心褶皱、脚趾并趾和先天性眼球震颤。缺失的断点是非典型的,位于先前表征的低拷贝重复序列(69838-72897Mb)之外。基因分型数据显示该缺失发生在父本染色体上。在 AGRE 家庭中,没有观察到较大的 15q24 缺失。
从目前和以往的研究来看,15q24 区域的缺失是 ASD 的罕见病因,在通过 ASD 确定的个体中,其频率估计为 0.1%至 0.2%,尽管在散发性病例中,该比例可能更高。这些发生率与通过智力障碍和先天性异常确定的不明原因智力障碍患者的发生率约为 0.3%相比较。这种非典型的缺失将综合征的最小区间从 1.75Mb 缩小到 766kb,涉及的基因数量减少(15 个对 38 个)。在大型 ASD 和智力障碍样本中对 15q24 区间的基因测序,可能会鉴定出这些疾病发展中具有重要病因意义的突变。
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