Villard L, Kpebe A, Cardoso C, Chelly P J, Tardieu P M, Fontes M
INSERM U491, Faculté de Médecine La Timone, Marseille, France.
Neurology. 2000 Oct 24;55(8):1188-93. doi: 10.1212/wnl.55.8.1188.
The authors report a family in which two boys had severe neonatal encephalopathy of unknown origin. They both presented with the same condition and died of severe apnea before they were 1 year old. Their sister has a classic form of Rett syndrome.
Because mutations in the methyl-CpG-binding protein 2 (MECP2) gene have been identified in 70 to 80% of the sporadic cases of Rett syndrome, the authors looked for a mutation in the MECP2 gene in this family.
The authors identified a missense mutation (T158M) in the affected girl and subsequently showed that one of her affected brothers, for whom DNA was available, carried the same mutation. The mother of the patients is a carrier of the T158M mutation. X-chromosome inactivation studies showed that the mother has a completely skewed X-chromosome inactivation pattern that favors the expression of the normal allele; this explains why she does not exhibit any phenotypic manifestation. In addition, the MECP2 mutation appeared on the grandpaternal X chromosome in this family.
An MECP2 mutation can be identified in boys, even though they do not present a Rett syndrome phenotype.
作者报告了一个家庭,其中两个男孩患有病因不明的严重新生儿脑病。他们都表现出相同的病症,并在1岁前死于严重呼吸暂停。他们的妹妹患有典型形式的雷特综合征。
由于在70%至80%的散发性雷特综合征病例中已发现甲基化CpG结合蛋白2(MECP2)基因突变,作者在这个家庭中寻找MECP2基因的突变。
作者在患病女孩中鉴定出一个错义突变(T158M),随后发现她的一个患病兄弟(有可用的DNA)携带相同的突变。患者的母亲是T158M突变的携带者。X染色体失活研究表明,母亲具有完全偏向的X染色体失活模式,有利于正常等位基因的表达;这解释了为什么她没有表现出任何表型表现。此外,该家庭中的MECP2突变出现在祖父的X染色体上。
即使男孩没有表现出雷特综合征表型,也可以在他们身上鉴定出MECP2突变。
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