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首页> 外文期刊>Journal of human genetics >Severe phenotypes in a Charcot-Marie-Tooth 1A patient with PMP22 triplication
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Severe phenotypes in a Charcot-Marie-Tooth 1A patient with PMP22 triplication

机译:Charcot-Marie-Tooth 1A患有PMP22三联的患者中的严重表型

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摘要

Charcot-Marie-Tooth disease (CMT) is a genetically and clinically heterogeneous hereditary motor and sensory neuropathy signified by a distal symmetric polyneuropathy. The most frequent subtype is type 1A (CMT1A) caused by duplication in chromosome 17p12 that includes PMP22. This study reports a woman with a family history of CMT1A due to PMP22 duplication. However, she presented with a more severe phenotype than her sibling or ancestors and was found to have a PMP22 triplication instead of the duplication. This was caused by de novo mutation on her affected mother's duplication chromosome. Her lower limb magnetic resonance imaging revealed severe diffused atrophy and fatty replacement. However, her affected sister with typical PMP22 duplication showed almost intact lower limb. Triplication patient's median motor nerve conduction velocity was far lower compared with her sister. Her onset age was faster (8 years) than her sister (42 years). CMT1A triplication might be generated by a female-specific chromosomal rearrangement mechanism that is different from the frequent paternal-originated CMT1A duplication. It also suggests that the wide phenotypic variation of CMT1A might be partly caused by unstable genomic rearrangement, including PMP22 triplication.
机译:Charcot-Marie-Tooth病(CMT)是一种遗传和临床异质性遗传运动和感觉神经病,以远端对称性多发性神经病为标志。最常见的亚型是1A型(CMT1A),由包含PMP22的17p12号染色体重复引起。这项研究报告了一名女性,由于PMP22复制而具有CMT1A家族史。然而,她表现出比同胞或祖先更严重的表型,并且被发现具有PMP22三联而不是重复。这是由她受影响的母亲的复制染色体上的从头突变引起的。她的下肢磁共振成像显示严重弥漫性萎缩和脂肪替代。但是,她患病的妹妹具有典型的PMP22复制,显示下肢几乎完整。三胞胎患者的中位运动神经传导速度远低于其姐姐。她的发病年龄比她的姐姐(42岁)快(8岁)。 CMT1A重复可能是由女性特有的染色体重排机制产生的,该机制与父系起源频繁的CMT1A重复不同。这也表明,CMT1A的广泛表型变异可能部分是由于不稳定的基因组重排,包括PMP22三重复。

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