Foley C, Roberts K, Tchrakian N, Morgan T, Fryer A, Robertson S P, Tubridy N
Department of Neurology, St. Vincent's University Hospital, Dublin, Ireland.
Mol Syndromol. 2010 Sep;1(3):121-126. doi: 10.1159/000320184. Epub 2010 Sep 14.
Melnick-Needles syndrome (MNS) is a rare X-linked bone dysplasia characterised by facial dysmorphology and radiographic abnormalities [Melnick and Needles, 1966;97:39-48]. Previously, all published cases of MNS were associated with only 4 mutations [Robertson et al., 2003;33:487-491; Santos et al., 2010;152A:726-731], all localised within exon 22 of FLNA, the gene encoding the cytoskeletal protein filamin A. Here we report 3 new mutations in FLNA that are associated with MNS. One affected member of the first family with the mutation p.Y1229S presented with a stroke while this patient's daughter, previously known to be affected from a young age, developed multiple sclerosis. A second unrelated patient with a typical phenotype is shown to have the mutation c.1054G>T (p.G352W) within exon 7 of FLNA. A third individual with an atypical presentation but radiological findings very similar to those seen in classic MNS has a deletion likely to affect residues within repeat domain 14. These findings indicate that the mutational spectrum for MNS is wider than previously appreciated and has implications for genetic testing strategies employed to confirm a diagnosis of this rare disorder.
梅尼克-尼德尔斯综合征(MNS)是一种罕见的X连锁骨发育不良,其特征为面部畸形和影像学异常[梅尼克和尼德尔斯,1966;97:39 - 48]。此前,所有已发表的MNS病例仅与4种突变相关[罗伯逊等人,2003;33:487 - 491;桑托斯等人,2010;152A:726 - 731],所有这些突变都位于编码细胞骨架蛋白细丝蛋白A的FLNA基因的第22外显子内。在此,我们报告了与MNS相关的FLNA基因中的3种新突变。第一个家族中有一名携带p.Y1229S突变的患病成员出现了中风,而该患者的女儿从小就已知患病,后来发展为多发性硬化症。第二名无亲缘关系的典型表型患者被证明在FLNA基因的第7外显子中有c.1054G>T(p.G352W)突变。第三名表现不典型但影像学表现与经典MNS非常相似的个体有一个缺失,可能影响重复结构域14内的残基。这些发现表明,MNS的突变谱比之前认识到的更广泛,这对用于确诊这种罕见疾病的基因检测策略具有重要意义。
