西班牙早发性阿尔茨海默病中早老素和淀粉样前体蛋白基因突变的频率。

Frequency of mutations in the presenilin and amyloid precursor protein genes in early-onset Alzheimer disease in Spain.

作者信息

Lleó Alberto, Blesa Rafael, Queralt Rosa, Ezquerra Mario, Molinuevo José L, Peña-Casanova Jordi, Rojo Ana, Oliva Rafael

机构信息

Neurology Service, Hospital Clínic, Institut d' Investigacions Biomediques Agusti Pi i Sunyer, Barcelona, Spain.

出版信息

Arch Neurol. 2002 Nov;59(11):1759-63. doi: 10.1001/archneur.59.11.1759.

DOI:10.1001/archneur.59.11.1759

PMID:12433263

Abstract

BACKGROUND

The relative contribution of mutations in the presenilin (PSEN) and amyloid precursor protein genes to autosomal dominant and other early-onset Alzheimer disease (AD) cases is not well established.

OBJECTIVES

To clarify the respective contribution of the amyloid precursor protein and PSEN mutations to autosomal dominant AD and to determine its contribution to sporadic and familial nonautosomal dominant early-onset AD and familial late-onset AD in a referral-based Spanish population.

SUBJECTS AND METHODS

Ninety-four patients with AD (60 with early-onset AD and 34 with late-onset AD) from 82 independent families were studied. According to the family history, patients were classified into the following groups: autosomal dominant, familial nonautosomal dominant, and sporadic. Mutational analysis of the coding regions of the amyloid precursor protein, presenilin 1, and presenilin 2 was performed in all patients. Apolipoprotein E was also genotyped.

RESULTS

Of the 60 early-onset cases, 44 from 36 families had a positive family history (11 with autosomal dominant AD and 25 with familial nonautosomal dominant AD) and 16 were sporadic. The frequency of mutations was 54.6% (6/11) among the autosomal dominant group, 6.2% (1/16) among the sporadic group, and 4% (1/25) among the familial nonautosomal dominant AD group. Most PSEN mutations (92%) would have been detected using a cutoff age of 58 years. The apolipoprotein E epsilon4 allele frequency was increased among early-onset AD without PSEN mutations.

CONCLUSIONS

More than half of the families with autosomal dominant early-onset AD can be explained by coding mutations in the PSEN genes. In the familial and sporadic early-onset groups mutations are rare. When family history is unavailable, an age of 58 years may be used as a cutoff point for genetic analysis. The increased apolipoprotein E epsilon4 allele in patients without PSEN mutations confirms that it is an important risk factor in the cause of non-PSEN early-onset AD.

摘要

背景

早老素（PSEN）和淀粉样前体蛋白基因突变对常染色体显性及其他早发型阿尔茨海默病（AD）病例的相对贡献尚未明确。

目的

在一个基于转诊的西班牙人群中，阐明淀粉样前体蛋白和PSEN突变对常染色体显性AD的各自贡献，并确定其对散发性和家族性非常染色体显性早发型AD以及家族性晚发型AD的贡献。

研究对象与方法

对来自82个独立家庭的94例AD患者（60例早发型AD和34例晚发型AD）进行研究。根据家族史，患者被分为以下几组：常染色体显性、家族性非常染色体显性和散发性。对所有患者进行淀粉样前体蛋白、早老素1和早老素2编码区的突变分析。同时对载脂蛋白E进行基因分型。

结果

在60例早发型病例中，36个家庭的44例有阳性家族史（11例常染色体显性AD和25例家族性非常染色体显性AD），16例为散发性。常染色体显性组突变频率为54.6%（6/11），散发性组为6.2%（1/16），家族性非常染色体显性AD组为4%（1/25）。使用截止年龄58岁，大多数PSEN突变（92%）本可被检测到。在无PSEN突变的早发型AD患者中，载脂蛋白Eε4等位基因频率升高。