Kodaganur Srinivas Gopinath, Kapoor Saketh, Veerappa Avinash M, Tontanahal Sagar Jagannath, Sarda Astha, Yathish S, Prakash D Ravi, Kumar Arun
Minto Eye Hospital, Bangalore Medical College and Research Institute, Bangalore India.
Mol Vis. 2013 Aug 2;19:1694-706. Print 2013.
Congenital hereditary endothelial dystrophy 2 (CHED2) is an autosomal recessive disorder caused by mutations in the solute carrier family 4, sodium borate transporter, member 11 (SLC4A11) gene. The purpose of this study was to identify the genetic cause of CHED2 in six Indian families and catalog all known mutations in the SLC4A11 gene.
Peripheral blood samples were collected from individuals of the families with CHED2 and used in genomic DNA isolation. PCR primers were used to amplify the entire coding region including intron-exon junctions of SLC4A11. Amplicons were subsequently sequenced to identify the mutations.
DNA sequence analysis of the six families identified four novel (viz., p.Thr262Ile, p.Gly417Arg, p.Cys611Arg, and p.His724Asp) mutations and one known p.Arg869His homozygous mutation in the SLC4A11 gene. The mutation p.Gly417Arg was identified in two families.
This study increases the mutation spectrum of the SLC4A11 gene. A review of the literature showed that the total number of mutations in the SLC4A11 gene described to date is 78. Most of the mutations are missense, followed by insertions-deletions. The present study will be helpful in genetic diagnosis of the families reported here.
先天性遗传性内皮营养不良2型(CHED2)是一种常染色体隐性疾病,由溶质载体家族4成员11(SLC4A11)基因中的突变引起。本研究旨在确定六个印度家庭中CHED2的遗传病因,并梳理SLC4A11基因中所有已知的突变。
从患有CHED2的家庭个体中采集外周血样本,用于基因组DNA分离。使用聚合酶链反应(PCR)引物扩增包括SLC4A11基因内含子-外显子连接区在内的整个编码区域。随后对扩增产物进行测序以识别突变。
对这六个家庭的DNA序列分析在SLC4A11基因中鉴定出四个新突变(即p.Thr262Ile、p.Gly417Arg、p.Cys611Arg和p.His724Asp)以及一个已知的p.Arg869His纯合突变。p.Gly417Arg突变在两个家庭中被鉴定出。
本研究增加了SLC4A11基因的突变谱。文献综述表明,迄今为止描述的SLC4A11基因中的突变总数为78个。大多数突变是错义突变,其次是插入-缺失突变。本研究将有助于对本文报道的家庭进行基因诊断。
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