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Genetics of dementia in a Finnish cohort

机译:芬兰队列中痴呆症的遗传学

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Alzheimer's disease (AD) and frontotemporal dementia (FTD) are the two most common neurodegenerative dementias. Variants in APP, PSEN1 and PSEN2 are typically linked to early-onset AD, and several genetic risk loci are associated with late-onset AD. Inherited FTD can be caused by hexanucleotide expansions in C9oif72, or variants in GRN, MAPT or CHMP2B. Several other genes have also been linked to FTD or FTD with motor neuron disease. Here we describe a cohort of 60 Finnish families with possible inherited dementia. Our aim was to clarify the genetic background of dementia in this cohort by analysing both known dementia-associated genes (APOE, APP, C9ORF72, GRN, PSEN1 and PSEN2) and searching for rare or novel segregating variants with exome sequencing. C9oif72 repeat expansions were detected in 12 (20%) of the 60 families, including, in addition to FTD, a family with neuropathologically verified AD. Twelve families (10 with AD and 2 with FTD) with representative samples from affected and unaffected subjects and without C9oif72 expansions were selected for whole-exome sequencing. Exome sequencing did not reveal any variants that could be regarded unequivocally causative, but revealed potentially damaging variants in UNCJ3C and MARCH4.
机译:阿尔茨海默病(AD)和额定颞痴呆症(FTD)是两种最常见的神经变性痴呆症。 APP中的变体,PSEN1和PSEN2通常与早期发作AD相关联,几个遗传风险基因座与晚发布的广告相关。遗传的FTD可以由C9OIF72中的己核苷酸扩展或GRN,MAPT或CHMP2B中的变体引起。其他几种基因也与电动神经元疾病的FTD或FTD相关联。在这里,我们描述了60个芬兰家族的队列,具有可能遗传的痴呆症。我们的目的是通过分析已知的痴呆相关基因(Apoe,App,C9orf72,Grn,Psen1和Psen2)来阐明该队列中痴呆症的遗传背景,并寻找具有外壳测序的稀有或新的偏析变体。 C9OIF72在60个家庭的12名(20%)中检测到C9OIF72重复扩展,包括除FTD,一个具有神经病理学验证的广告的家庭。为全外exome测序选择了来自受影响和未受影响的受试者的代表样品和不受C9OIF72扩展的12个家庭(带有AD和FTD的ad和FTD)。 Exome测序没有揭示任何可能认为明确造成的变体,但在UNCJ3C和3月4日揭示了潜在的破坏性变种。

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