Wang Juan, Liu Jinling, Zhang Qingjiong
State Key Laboratory of Ophthalmology, Zhongshan Ophthalmic Center, Sun Yat-Sen University, Guangzhou, China.
Mol Vis. 2007 Jan 26;13:108-13.
Blepharophimosis-ptosis-epicanthus inversus syndrome (BPES) is an autosomal dominant disorder where eyelid malformation associated with (type I) or without (type II) premature ovarian failure (POF). It is ascribed to mutations in the forkhead transcriptional factor2 (FOXL2) gene. The purpose of this study is to identify mutations in FOXL2 of Chinese patients with BPES.
Genomic DNA was prepared from leucocytes of peripheral venous blood. The coding regions and nearby intron sequences of FOXL2 were analyzed by cycle and cloning sequencing.
Four mutations in FOXL2 were identified in six families, including c.241T>C, c.650C>G, c.804dupC, and c.672_701dup. Of the four, the c.241T>C and c.650C>G were novel and would result in missense changes of the encoded proteins, i.e., p.Tyr81His and p.Ser217Cys, respectively. The c.672_701dup (p.Ala224_Ala234dup) was detected in three families, indicating a mutation hotspot. The c.804dupC (p.Gly269ArgfsX265) mutation was found in one family.
Our results expand the spectrum of FOXL2 mutations and confirm the mutation hotspot in FOXL2.
睑裂狭小-上睑下垂-内眦赘皮综合征(BPES)是一种常染色体显性疾病,伴有(I型)或不伴有(II型)卵巢早衰(POF)的眼睑畸形。它归因于叉头转录因子2(FOXL2)基因的突变。本研究的目的是鉴定中国BPES患者中FOXL2的突变。
从外周静脉血白细胞中提取基因组DNA。通过循环测序和克隆测序分析FOXL2的编码区和附近的内含子序列。
在6个家系中鉴定出FOXL2的4种突变,包括c.241T>C、c.650C>G、c.804dupC和c.672_701dup。其中,c.241T>C和c.650C>G是新发现的突变,将分别导致编码蛋白的错义改变,即p.Tyr81His和p.Ser217Cys。c.672_701dup(p.Ala224_Ala234dup)在3个家系中被检测到,表明这是一个突变热点。c.804dupC(p.Gly269ArgfsX265)突变在1个家系中被发现。
我们的结果扩展了FOXL2突变谱,并证实了FOXL2中的突变热点。
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