Lin Hui-Chi, Lin Chin-Hsien, Chen Pei-Lung, Cheng Shih-Jung, Chen Pei-Hao
Department of Neurology, MacKay Memorial Hospital, No. 92, Sec. 2, Zhongshan N. Rd., Zhongshan Dist, Taipei City, 10449, Taiwan.
Department of Neurology, National Taiwan University Hospital, No. 7, Chung-Shan South Road, Taipei, 100, Taiwan.
BMC Neurol. 2017 Sep 18;17(1):186. doi: 10.1186/s12883-017-0966-3.
Frontotemporal degeneration (FTD) is a clinically and genetically heterogeneous neurodegenerative disorder characterized by deficits in executive function that frequently overlaps with parkinsonism and motor neuron disorders. Several genes have been identified to cause autosomal dominant forms of FTD, including the gene coding for the protein associated with microtubule tau (MAPT). While most reported pathogenic mutations in MAPT occur in exons 9-13, few families have been reported with mutations outside of this region. Herein, we report a first Taiwanese family having the exon 1 p.Arg5His mutation in MAPT with intrafamilial phenotype heterogeneity.
A 63-year-old man presented with progressive non-fluent speech and impaired memory for 3 years. He then developed apraxia, myoclonus and parkinsonism feature at his right hand. Extensive neurologic and neurocognitive examination lead to a diagnosis of FTD mixed with corticobasal syndrome. Magnetic resonance imaging revealed asymmetric atrophy in the left frontal and temporal lobes and single-photon emission computed tomography indicated decreased metabolism in the same areas as well as the left basal ganglia. The patient's mother had been diagnosed with amyotrophic lateral sclerosis (ALS) at the age of 60 and was deceased 10 years later due to respiratory failure. The patient's younger sister had persistent depressive disorder in her early forties and did not have any prominent cognitive or motor dysfunctions. We performed genetic analysis applying a targeted next generation sequencing (NGS) panel covering MAPT, GRN, VCP, FUS, CHMP2B, and TARDBP on the proband, followed by Sanger sequencing of candidate genes in eight family members. Hexanucleotide repeat expansion of C9Orf72 was determined by repeat-primed PCR. We identified a missense mutation in exon 1 of MAPT gene, c.14G > A (p.R5H), which was previously reported in only two Japanese patients in a literature review. This substitution co-segregated with the disease phenotypes in the family.
This is the first report of the occurrence of the MAPT p.R5H mutation in the Taiwanese population. Our findings extend the current knowledge of phenotypic heterogeneity among family members carrying the MAPT p.R5H mutation.
额颞叶变性(FTD)是一种临床和基因异质性神经退行性疾病,其特征为执行功能缺陷,常与帕金森综合征和运动神经元疾病重叠。已确定多个基因可导致常染色体显性形式的FTD,包括编码与微管tau蛋白(MAPT)相关的蛋白质的基因。虽然大多数报道的MAPT致病突变发生在外显子9 - 13,但很少有家族报道在此区域外存在突变。在此,我们报告一个首例台湾家族,其MAPT基因外显子1存在p.Arg5His突变,且家族内存在表型异质性。
一名63岁男性,出现进行性非流畅性言语及记忆力减退3年。随后右手出现失用症、肌阵挛及帕金森综合征特征。广泛的神经学和神经认知检查导致诊断为FTD合并皮质基底节综合征。磁共振成像显示左侧额叶和颞叶不对称萎缩,单光子发射计算机断层扫描显示相同区域以及左侧基底节代谢降低。患者母亲在60岁时被诊断为肌萎缩侧索硬化(ALS),10年后因呼吸衰竭去世。患者的妹妹在四十出头时患有持续性抑郁症,无任何明显的认知或运动功能障碍。我们对先证者应用覆盖MAPT、GRN、VCP、FUS、CHMP2B和TARDBP的靶向二代测序(NGS)面板进行基因分析,随后对8名家族成员的候选基因进行桑格测序。通过重复引物PCR确定C9Orf72的六核苷酸重复扩增。我们在MAPT基因外显子1中鉴定出一个错义突变,c.14G > A(p.R5H),在文献综述中此前仅在两名日本患者中报道过。该替换与家族中的疾病表型共分离。
这是台湾人群中MAPT p.R5H突变发生情况的首例报告。我们的发现扩展了目前对携带MAPT p.R5H突变的家族成员中表型异质性的认识。
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