Gender and age modify the association between APOE and AD-related neuropathology.

Ghebremedhin E; Schultz C; Thal DRRub UOhm TGBraak EBraak H

首页> 外文期刊>Neurology: Official Journal of the American Academy of Neurology >Gender and age modify the association between APOE and AD-related neuropathology.

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Gender and age modify the association between APOE and AD-related neuropathology.

机译：性别和年龄修改APOE之间的关系和AD-related神经病理学。

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OBJECTIVE: To assess the impact of apolipoprotein E (APOE) polymorphism on AD-related neurofibrillary tangle (NFT) formation and senile plaques (SP). METHODS: A sample of 729 routine autopsy brains (359 men, 370 women; age range, 60 to 99 years) was investigated. All brains were classified neuropathologically according to a procedure permitting differentiation of six NFT stages and three SP stages. APOE genotyping was performed on all cases. RESULTS: The epsilon4 allele of APOE was associated not only with SP (p or =80 years (p or =80 years of age (p = 0.063). By comparison, men showed an association in both age categories (p = 0.001 and p = 0.001). CONCLUSION: The results confirm the association between the epsilon4 allele and both types of AD-related lesions and show that this association is differentially modified by age and gender.

机译：目的:评估载脂蛋白的影响AD-related E (APOE)多态性神经原纤维缠结形成和老年(非功能性测试)斑块(SP)。解剖大脑(359名男性,370名女性;99年)进行了研究。显示神经病理分类过程允许分化的六个非功能性测试阶段和三个SP阶段。在所有情况下执行。不仅与SP的APOE等位基因关联(p = 80年(p = 80岁(p= 0.063)。协会在这两个类别(p = 0.001和年龄p = 0.001)。epsilon4等位基因和两个之间的联系类型的AD-related病变和显示协会是由年龄和不同的修改性别。

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来源
《Neurology: Official Journal of the American Academy of Neurology》 |2001年第12期|1696-1701|共6页
作者
Ghebremedhin E; Schultz C; Thal DRRub UOhm TGBraak EBraak H;
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作者单位

Department of Clinical Neuroanatomy, J.W. Goethe-University, Frankfurt, Germany. Ghebremedhin;

asteur.fr;

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正文语种英语
中图分类神经病学;
关键词
Apolipoproteins E; Age Factor; Association (Psychology)Alzheimer DiseaseNeurofibrillary TanglesGenderNeuropathologyCerebrum;

机译：载脂蛋白E;年龄因素;协会(心理学)DiseaseNeurofibrillary老年痴呆症;

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Gender and age modify the association between APOE and AD-related neuropathology.

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