GeneDx, Gaithersburg, Maryland, USA.
Genet Med. 2012 Jun;14(6):594-603. doi: 10.1038/gim.2011.65. Epub 2012 Mar 1.
Mendelian disorders are most commonly caused by mutations identifiable by DNA sequencing. Exonic deletions and duplications can go undetected by sequencing, and their frequency in most Mendelian disorders is unknown.
We designed an array comparative genomic hybridization (CGH) test with probes in exonic regions of 589 genes. Targeted testing was performed for 219 genes in 3,018 patients. We demonstrate for the first time the utility of exon-level array CGH in a large clinical cohort by testing for 136 autosomal dominant, 53 autosomal recessive, and 30 X-linked disorders.
Overall, 98 deletions and two duplications were identified in 53 genes, corresponding to a detection rate of 3.3%. Approximately 40% of positive findings were deletions of only one or two exons. A high frequency of deletions was observed for several autosomal dominant disorders, with a detection rate of 2.9%. For autosomal recessive disorders, array CGH was usually performed after a single mutation was identified by sequencing. Among 138 individuals tested for recessive disorders, 10.1% had intragenic deletions. For X-linked disorders, 3.5% of 313 patients carried a deletion or duplication.
Our results demonstrate that exon-level array CGH provides a robust option for intragenic copy number analysis and should routinely supplement sequence analysis for Mendelian disorders.
孟德尔氏疾病通常由可通过 DNA 测序识别的突变引起。外显子缺失和重复可能会被测序遗漏,并且它们在大多数孟德尔氏疾病中的频率尚不清楚。
我们设计了一种包含 589 个基因外显子区域探针的阵列比较基因组杂交(CGH)测试。对 3018 名患者的 219 个基因进行了靶向测试。我们首次通过测试 136 种常染色体显性、53 种常染色体隐性和 30 种 X 连锁疾病,证明了外显子水平阵列 CGH 在大型临床队列中的实用性。
总体而言,在 53 个基因中发现了 98 个缺失和两个重复,对应于 3.3%的检测率。大约 40%的阳性结果是仅缺失一个或两个外显子。几种常染色体显性疾病的缺失频率较高,检测率为 2.9%。对于常染色体隐性疾病,在通过测序确定单个突变后通常会进行阵列 CGH。在对 138 名接受隐性疾病测试的个体中,有 10.1%存在基因内缺失。对于 X 连锁疾病,313 名患者中有 3.5%携带缺失或重复。
我们的结果表明,外显子水平阵列 CGH 为基因内拷贝数分析提供了一种强大的选择,并且应该常规补充孟德尔氏疾病的序列分析。
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