Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, TX, USA.
Neurogenetics. 2010 Oct;11(4):465-70. doi: 10.1007/s10048-010-0247-4. Epub 2010 Jun 9.
The X-linked form of Charcot-Marie-Tooth disease (CMTX) is the second most common form of this genetically heterogeneous inherited peripheral neuropathy. CMT1X is caused by mutations in the GJB1 gene. Most of the mutations causative for CMT1X are missense mutations. In addition, a few disease causative nonsense mutations and frameshift deletions that lead to truncated forms of the protein have also been reported to be associated with CMT1X. Previously, there have been reports of patients with deletions of the coding sequence of GJB1; however, the size and breakpoints of these deletions were not assessed. Here, we report five patients with deletions that range in size from 12.2 to 48.3 kb and that completely eliminate the entire coding sequence of the GJB1 gene, resulting in a null allele for this locus. Analyses of the breakpoints of these deletions showed that they are nonrecurrent and that they can be generated by different mechanisms. In addition to PMP22, GJB1 is the second CMT gene for which both point mutations and genomic rearrangements can cause a neuropathy phenotype, stressing the importance of CMT as a genomic disorder.
X 连锁型遗传性运动感觉神经病(Charcot-Marie-Tooth disease,CMT)是遗传异质性周围神经病中第二常见的类型。CMT1X 是由 GJB1 基因突变引起的。导致 CMT1X 的大多数突变是错义突变。此外,也有一些疾病相关的无义突变和移码缺失导致截短的蛋白形式,这些也被报道与 CMT1X 相关。先前有报道称 GJB1 编码序列缺失,但这些缺失的大小和断点并未得到评估。在这里,我们报告了五例缺失大小在 12.2 到 48.3kb 之间的患者,这些缺失完全消除了 GJB1 基因的整个编码序列,导致该基因座的无效等位基因。对这些缺失断点的分析表明,它们是非重复的,可以通过不同的机制产生。除了 PMP22 之外,GJB1 是第二个既可以由点突变又可以由基因组重排引起周围神经病表型的 CMT 基因,这强调了 CMT 作为一种基因组疾病的重要性。
