Zhang Qingjiong, Xiao Xueshan, Li Shiqiang, Guo Xiangming
State Key Laboratory of Ophthalmology, Zhongshan Ophthalmic Center, Sun Yat-sen University, Guangzhou, China.
Mol Vis. 2007 Aug 3;13:1375-8.
To identify mutations causing X-linked congenital motor nystagmus (XL-CMN) in Chinese families.
Genomic DNA was prepared from peripheral blood leukocytes. Cycle sequencing was used to detect the sequence variation of the FERM domain containing 7 (FRMD7) gene, where mutations have been identified recently to associate with XL-CMN.
Sequencing of the coding and the adjacent intron regions of FRMD7 identified mutations in four families with XL-CMN, c.41-43delAGA (p.Lys14del) in exon 1, c.70G>A (p.Gly24Arg) in exon 2, c.436C>T (p.Arg146Trp) in exon 6, and c.685C>T (p.Arg229Cys) in exon 8, respectively, where the last two were novel. These mutations were not detected in 196 normal controls. In the two families with X-linked recessive CMN, females carrying a heterozygous mutation in FRMD7 did not have any sign of nystagmus.
Our results provide additional evidence for mutations in FRMD7 as a common cause of XL-CMN and expand its mutation spectrum. CMN in a Chinese family with pure X-linked recessive pattern, previously mapped to Xq23-q27, is associated with the c.41-43delAGA mutation in FRMD7.
鉴定中国家系中导致X连锁先天性眼球震颤(XL-CMN)的突变。
从外周血白细胞中提取基因组DNA。采用循环测序法检测含FERM结构域7(FRMD7)基因的序列变异,该基因最近被鉴定出与XL-CMN相关。
对FRMD7的编码区和相邻内含子区域进行测序,在4个XL-CMN家系中鉴定出突变,分别为外显子1中的c.41-43delAGA(p.Lys14del)、外显子2中的c.70G>A(p.Gly24Arg)、外显子6中的c.436C>T(p.Arg146Trp)和外显子8中的c.685C>T(p.Arg229Cys),其中后两个突变为新发现的突变。在196名正常对照中未检测到这些突变。在两个X连锁隐性CMN家系中,携带FRMD7杂合突变的女性没有任何眼球震颤迹象。
我们的结果为FRMD7突变是XL-CMN的常见病因提供了更多证据,并扩大了其突变谱。一个先前定位于Xq23-q27的具有纯X连锁隐性模式的中国家系中的CMN与FRMD7基因的c.41-43delAGA突变相关。
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