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认知正常的载脂蛋白E-ε4纯合子的临床前记忆衰退。

Preclinical memory decline in cognitively normal apolipoprotein E-epsilon4 homozygotes.

作者信息

Caselli R J, Graff-Radford N R, Reiman E M, Weaver A, Osborne D, Lucas J, Uecker A, Thibodeau S N

机构信息

Department of Neurology, Mayo Clinic Scottsdale, AZ 85259, USA.

出版信息

Neurology. 1999 Jul 13;53(1):201-7. doi: 10.1212/wnl.53.1.201.

DOI:10.1212/wnl.53.1.201
PMID:10408560
Abstract

OBJECTIVE

To determine, in a cross-sectional evaluation of nondemented individuals, if age-related memory decline is influenced by apolipoprotein E (apoE) genotype.

BACKGROUND

The apoE-4 allele is an important risk factor for AD. PET in cognitively normal apoE-4 carriers (mean age, 56 years) shows reduced cerebral metabolism suggestive of very early AD that precedes clinically evident memory loss or MRI-based hippocampal atrophy.

METHODS

Tests of immediate and delayed recall (primary outcome measures) and other neuropsychological measures (secondary outcome measures) were given to three genetically defined groups of cognitively normal individuals (age, 49 to 69 years) including apoE-4 homozygotes (n = 25), apoE-4 heterozygotes (n = 25, all epsilon3/4), and apoE-4 noncarriers (n = 50). Groups were matched for age, gender, and educational background. Cross-sectional comparisons between the genetic subgroups of the relationship between age and test score were performed for each neuropsychological measure.

RESULTS

There were no intergroup differences in mean scores on any neuropsychological measure, but tests sensitive to immediate and delayed recall showed a significant negative correlation with age in the apoE-4 homozygote group relative to the noncarrier group.

CONCLUSION

Consistent with previous neuropsychological studies of early AD, this cross-sectional study suggests that age-related memory decline occurs earlier in cognitively healthy apoE-4 homozygotes than in apoE-4 heterozygotes and noncarriers, and precedes clinically detectable AD.

摘要

目的

在对非痴呆个体的横断面评估中,确定载脂蛋白E(apoE)基因型是否会影响与年龄相关的记忆衰退。

背景

apoE-4等位基因是阿尔茨海默病(AD)的一个重要风险因素。对认知正常的apoE-4携带者(平均年龄56岁)进行的正电子发射断层扫描(PET)显示,大脑代谢降低,提示在临床上明显的记忆丧失或基于磁共振成像(MRI)的海马萎缩之前就已出现非常早期的AD。

方法

对三组基因定义的认知正常个体(年龄49至69岁)进行即时和延迟回忆测试(主要结局指标)以及其他神经心理学测试(次要结局指标),这三组包括apoE-4纯合子(n = 25)、apoE-4杂合子(n = 25,均为ε3/4)和apoE-4非携带者(n = 50)。各组在年龄、性别和教育背景方面进行了匹配。对每项神经心理学测试,在各基因亚组之间进行年龄与测试分数关系的横断面比较。

结果

在任何神经心理学测试的平均分数上,各组之间均无差异,但相对于非携带者组,对即时和延迟回忆敏感的测试显示,apoE-4纯合子组中年龄与测试分数呈显著负相关。

结论

与先前关于早期AD的神经心理学研究一致,这项横断面研究表明,在认知健康的情况下,apoE-4纯合子中与年龄相关的记忆衰退比apoE-4杂合子和非携带者出现得更早,且早于临床上可检测到的AD。

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