Chen J-H, Qiu J, Chen H, Pang C P, Zhang M
1] Joint Shantou International Eye Center, Shantou University and the Chinese University of Hong Kong, Shantou, China [2] Department of Ophthalmology and Visual Sciences, the Chinese University of Hong Kong, Hong Kong, China.
Joint Shantou International Eye Center, Shantou University and the Chinese University of Hong Kong, Shantou, China.
Eye (Lond). 2014 Dec;28(12):1511-6. doi: 10.1038/eye.2014.158. Epub 2014 Oct 10.
Due to high genetic heterogeneity, to exclude known mutations and map novel mutations in autosomal dominant congenital cataract (ADCC) using conventional candidate gene screening requires laborious laboratory work. We attempted to use a cost-effective exome sequencing strategy to identify disease-causing mutations in an ADCC pedigree.
An ADCC pedigree affected by nuclear cataract and 200 unrelated senile cataract controls were recruited and given comprehensive ophthalmic examination. Whole exome of the proband of the family was captured by the Illumina TruSeq Exome Enrichment Kit, followed by sequencing using Illumina HiSeq 2000 sequencer. Validation was performed by direct sequencing.
The whole exome, including all exons of known ADCC disease-causing genes, was screened for possible disease-causing mutations. A recurrent missense mutation c.773C>T (p.S258F) in exon 2 of the gap junction protein alpha 8 gene (GJA8) was identified in the proband with nuclear cataract. The result was confirmed by direct sequencing. The mutation showed complete co-segregation with the disease phenotype in the family but was not observed in unrelated unaffected controls.
By successfully sequencing whole exome of only one proband and identifying a GJA8 mutation in one ADCC pedigree, the current study demonstrated that exome sequencing could serve as a rapid, robust, and cost-effective approach in clinical diagnosis and disease-causing gene discovery for ADCC.
由于高度的遗传异质性,使用传统的候选基因筛查来排除常染色体显性先天性白内障(ADCC)中的已知突变并定位新突变需要繁琐的实验室工作。我们尝试使用一种经济高效的外显子组测序策略来鉴定一个ADCC家系中的致病突变。
招募一个受核性白内障影响的ADCC家系和200名无血缘关系的老年性白内障对照者,并对他们进行全面的眼科检查。使用Illumina TruSeq外显子组富集试剂盒捕获该家系先证者的整个外显子组,随后使用Illumina HiSeq 2000测序仪进行测序。通过直接测序进行验证。
对整个外显子组,包括已知ADCC致病基因的所有外显子,进行可能致病突变的筛查。在先证者的核性白内障中鉴定出缝隙连接蛋白α8基因(GJA8)第2外显子中的一个复发性错义突变c.773C>T(p.S258F)。该结果通过直接测序得到证实。该突变在家族中与疾病表型完全共分离,但在无血缘关系的未受影响对照者中未观察到。
通过仅对一名先证者的整个外显子组成功测序并在一个ADCC家系中鉴定出一个GJA8突变,本研究表明外显子组测序可作为ADCC临床诊断和致病基因发现的一种快速、可靠且经济高效的方法。
