Investigation of c9orf72 in 4 neurodegenerative disorders.

Zhengrui Xi, Lorne Zinman, Yakov Grinberg, Danielle Moreno, Christine Sato, Juan M Bilbao, Mahdi Ghani, Isabel Hernández, Agustín Ruiz, Mercè Boada, Francisco J Morón, Anthony E Lang, Connie Marras, Amalia Bruni, Rosanna Colao, Raffaele G Maletta, Gianfranco Puccio, Innocenzo Rainero, Lorenzo Pinessi, Daniela Galimberti, Karen E Morrison, Catriona Moorby, Joanne D Stockton, Mario Masellis, Sandra E Black, Lili-Naz Hazrati, Yan Liang, Jan van Haersma de With, Luis Fornazzari, Roque Villagra, Ricardo Rojas-Garcia, Jordi Clarimón, Richard Mayeux, Janice Robertson, Peter St George-Hyslop, Ekaterina Rogaeva
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Abstract

OBJECTIVE To estimate the allele frequency of C9orf72 (G4C2) repeats in amyotrophic lateral sclerosis (ALS), frontotemporal lobar degeneration (FTLD), Alzheimer disease (AD), and Parkinson disease (PD). DESIGN The number of repeats was estimated by a 2-step genotyping strategy. For expansion carriers, we sequenced the repeat flanking regions and obtained APOE genotypes and MAPT H1/H2 haplotypes. SETTING Hospitals specializing in neurodegenerative disorders. SUBJECTS We analyzed 520 patients with FTLD, 389 patients with ALS, 424 patients with AD, 289 patients with PD, 602 controls, 18 families, and 29 patients with PD with the LRRK2 G2019S mutation. MAIN OUTCOME MEASURE The expansion frequency. RESULTS Based on a prior cutoff (>30 repeats), the expansion was detected in 9.3% of patients with ALS, 5.2% of patients with FTLD, and 0.7% of patients with PD but not in controls or patients with AD. It was significantly associated with family history of ALS or FTLD and age at onset of FTLD. Phenotype variation (ALS vs FTLD) was not associated with MAPT, APOE, or variability in the repeat flanking regions. Two patients with PD were carriers of 39 and 32 repeats with questionable pathological significance, since the 39-repeat allele does not segregate with PD. No expansion or intermediate alleles (20-29 repeats) were found among the G2019S carriers and AD cases with TAR DNA-binding protein 43-positive inclusions. Surprisingly, the frequency of the 10-repeat allele was marginally increased in all 4 neurodegenerative diseases compared with controls, indicating the presence of an unknown risk variation in the C9orf72 locus. CONCLUSIONS The C9orf72 expansion is a common cause of ALS and FTLD, but not of AD or PD. Our study raises concern about a reliable cutoff for the pathological repeat number, which is important in the utility of genetic screening.

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研究 4 种神经退行性疾病中的 c9orf72。
目的 估计肌萎缩侧索硬化症(ALS)、额颞叶变性(FTLD)、阿尔茨海默病(AD)和帕金森病(PD)中C9orf72(G4C2)重复序列的等位基因频率。设计 通过两步基因分型策略估算重复序列的数量。对于扩增携带者,我们对重复侧翼区进行测序,并获得 APOE 基因型和 MAPT H1/H2 单倍型。地点 神经退行性疾病专科医院。受试者 我们分析了 520 名 FTLD 患者、389 名 ALS 患者、424 名 AD 患者、289 名 PD 患者、602 名对照组、18 个家庭和 29 名 LRRK2 G2019S 突变的 PD 患者。主要结果测量 扩增频率。结果 根据事先设定的截止值(30 次重复),在 9.3% 的 ALS 患者、5.2% 的 FTLD 患者和 0.7% 的 PD 患者中检测到扩增,但在对照组或 AD 患者中未检测到。它与 ALS 或 FTLD 家族史以及 FTLD 发病年龄有明显关联。表型变异(ALS 与 FTLD)与 MAPT、APOE 或重复侧翼区域的变异无关。两名帕金森病患者分别是 39 和 32 个重复序列的携带者,其病理意义值得怀疑,因为 39 个重复序列的等位基因不会与帕金森病发生分离。在G2019S携带者和TAR DNA结合蛋白43阳性包涵体的AD病例中,没有发现扩展等位基因或中间等位基因(20-29个重复序列)。令人惊讶的是,与对照组相比,10个重复等位基因在所有4种神经退行性疾病中的频率都略有增加,这表明C9orf72位点存在未知的风险变异。结论 C9orf72扩增是ALS和FTLD的常见病因,但不是AD或PD的常见病因。我们的研究引起了人们对病理重复数可靠临界值的关注,这对基因筛查的实用性非常重要。
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Archives of neurology
Archives of neurology 医学-临床神经学
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