携带tau蛋白N279K突变的家族的临床与遗传学研究（额颞叶痴呆伴帕金森综合征-17型）

Clinical and genetic studies of families with the tau N279K mutation (FTDP-17).

作者信息

Tsuboi Y, Baker M, Hutton M L, Uitti R J, Rascol O, Delisle M-B, Soulages X, Murrell J R, Ghetti B, Yasuda M, Komure O, Kuno S, Arima K, Sunohara N, Kobayashi T, Mizuno Y, Wszolek Z K

机构信息

Mayo Clinic, Jacksonville, FL 32224, USA.

出版信息

Neurology. 2002 Dec 10;59(11):1791-3. doi: 10.1212/01.wnl.0000038909.49164.4b.

DOI:10.1212/01.wnl.0000038909.49164.4b

PMID:12473774

Abstract

The tau N279K mutation was identified in four separately ascertained families in the United States, Japan, and France and in another recently discovered affected individual in Japan. The authors analyzed genealogical and clinical records and DNA samples. Average age at onset was 43 years; survival time was 7 years. All families exhibited similar clinical features, with parkinsonism, dementia, and supranuclear palsy uniformly seen. A founder effect indicated by a shared disease haplotype was seen only in two Japanese families. The N279K mutation can develop independently in different parts of the world.

摘要

在美国、日本和法国的四个独立确诊的家族以及日本另一位最近发现的患病个体中鉴定出了tau N279K突变。作者分析了系谱和临床记录以及DNA样本。平均发病年龄为43岁；存活时间为7年。所有家族均表现出相似的临床特征，均出现帕金森症、痴呆和核上性麻痹。仅在两个日本家族中发现了由共享疾病单倍型表明的奠基者效应。N279K突变可在世界不同地区独立发生。

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携带tau蛋白N279K突变的家族的临床与遗传学研究（额颞叶痴呆伴帕金森综合征-17型）

Clinical and genetic studies of families with the tau N279K mutation (FTDP-17).

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