Zhang Li, Wang Liming, Han Ruifang, Guan Lifang, Fan Baohong, Liu Mingmei, Ying Ming, Peng Hao, Li Ningdong
Henan Eye Institute, Henan Eye Hospital, Henan, People's Republic of China ; Tianjin Key Lab of Ophthalmology and Visual Science, Tianjin Eye Institute, Tianjin, People's Republic of China.
Mol Vis. 2013 Nov 16;19:2298-305. eCollection 2013.
To determine the genetic origin of disease in four Chinese families with blepharophimosis syndrome.
Four Han Chinese families with blepharophimosis syndrome were ascertained and patients underwent complete physical and ophthalmic examinations. Blood samples were collected and genomic DNA was extracted. Sequence analysis of the forkhead transcriptional factor 2 (FOXL2) gene was performed by direct sequencing and mutations were analyzed.
Three mutations in FOXL2 were found in four families, including c.672_701dup30 (p.Ala224_Ala234dup10), c.313C>A (p.N105H), and c.430G>T (p.R144W). The c.672_701dup30 (p.Ala224_Ala234dup10) mutation was reported previously and predicted to result in expansions of the polyalanine tract. The mutations of c.313C>A (p. N105H) and c.430G>T (p.R144W) are two novel missense mutations.
Our study further supports the view that the expansion of the polyalanine tract is the hotspot of mutations within FOXL2. The two novel missense mutations detected in this study will expand the mutation spectrum of the FOXL2 gene and contribute to the research on the molecular pathogenesis of FOXL2.
确定四个患有睑裂狭小综合征的中国家庭中疾病的遗传起源。
确定了四个患有睑裂狭小综合征的汉族家庭,患者接受了全面的体格和眼科检查。采集血样并提取基因组DNA。通过直接测序对叉头转录因子2(FOXL2)基因进行序列分析,并对突变进行分析。
在四个家庭中发现了FOXL2的三个突变,包括c.672_701dup30(p.Ala224_Ala234dup10)、c.313C>A(p.N105H)和c.430G>T(p.R144W)。c.672_701dup30(p.Ala224_Ala234dup10)突变先前已有报道,预计会导致多聚丙氨酸序列的扩增。c.313C>A(p.N105H)和c.430G>T(p.R144W)突变是两个新的错义突变。
我们的研究进一步支持了多聚丙氨酸序列扩增是FOXL2内突变热点的观点。本研究中检测到的两个新的错义突变将扩大FOXL2基因的突变谱,并有助于FOXL2分子发病机制的研究。
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