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Alzheimer’s Disease Genetic Risk Factor APOE-ε4 Also Affects Normal Brain Function

机译:阿尔茨海默氏病遗传危险因素APOE-ε4也影响正常脑功能

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摘要

APOE-ε4 is the strongest genetic risk factor for Alzheimer’s disease (AD), and is associated with an increase in the levels of amyloid deposition and an early age of onset. Recent data demonstrate that AD pathological changes occur decades before clinical symptoms, raising questions about the precise onset of the disease. Now a convergence of approaches in mice and humans has demonstrated that APOE-ε4 affects normal brain function even very early in life in the absence of gross AD pathological changes. Normal mice expressing APOE4 have task-specific spatial learning deficits, as well as reduced NMDAR-dependent signaling and structural changes to presynaptic and postsynaptic compartments in neurons, particularly in hippocampal regions. Young humans possessing APOE-ε4 are more adept than APOE-ε4 negative individuals at some behavioral tasks, and functional magnetic resonance imaging has shown that inheritance of APOE-ε4 has specific effects on medial temporal brain activities. These findings suggest that inheritance of APOE-ε4 causes life long changes to the brain that may be related to the late risk of AD. Several possible mechanisms of how APOE-ε4 could affect brain neurochemistry, structure, and function are reviewed.
机译:APOE-ε4是阿尔茨海默氏病(AD)的最强遗传危险因素,与淀粉样蛋白沉积水平增加和发病年龄提前有关。最新数据表明,AD病理变化发生在临床症状出现之前的几十年,从而引发了对该疾病确切发作的质疑。现在,小鼠和人类方法的融合表明,APOE-ε4甚至可以在生命初期很短的时间内就影响正常的大脑功能,而不会出现严重的AD病理变化。表达APOE4的正常小鼠具有特定于任务的空间学习缺陷,以及神经元(特别是在海马区)突触前和突触后区室的NMDAR依赖性信号传导和结构变化减少。具有APOE-ε4的年轻人在某些行为任务上比APOE-ε4阴性的人更为熟练,并且功能磁共振成像显示,APOE-ε4的遗传对内侧颞部大脑活动具有特定的影响。这些发现表明,APOE-ε4的遗传会导致大脑终生改变,这可能与晚期AD风险有关。本文对APOE-ε4如何影响大脑神经化学,结构和功能的几种可能机制进行了综述。

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