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APOE对人类颞叶新皮质突触蛋白的病前影响。

Premorbid effects of APOE on synaptic proteins in human temporal neocortex.

作者信息

Love Seth, Siew L Khai, Dawbarn David, Wilcock Gordon K, Ben-Shlomo Yoav, Allen Shelley J

机构信息

Department of Neuropathology, University of Bristol Institute of Clinical Neurosciences, Frenchay Hospital, Bristol BS16 1LE, UK.

出版信息

Neurobiol Aging. 2006 Jun;27(6):797-803. doi: 10.1016/j.neurobiolaging.2005.04.008. Epub 2005 Jun 23.

Abstract

APOE affects the risk of Alzheimer's disease (AD) and course of several other neurologic diseases. Experimental studies suggest that APOE influences synaptogenesis. We measured the concentration of two presynaptic proteins, synaptophysin and syntaxin 1, and also postsynaptic density-95 (PSD95), in superior temporal cortex from 42 AD and 160 normal brains, and determined the APOE genotypes. The concentration of both presynaptic proteins was approximately two-thirds lower in AD than normal brains and that of PSD95 one-third lower. No effect of APOE on synaptic proteins was found in advanced AD. However, in normal brain, epsilon4 was associated with lower concentrations of all three synaptic proteins and epsilon2 with significantly elevated PSD95 (p=0.03). A combined measure of synaptic proteins showed a significant linear decrease from epsilon2 through epsilon3 to varepsilon4 (p=0.01). APOE influences the concentration of synaptic proteins in normal superior temporal cortex and may thereby affect the response to injury, and the risk and outcome of a range of neurologic diseases.

摘要

载脂蛋白E(APOE)影响阿尔茨海默病(AD)的发病风险以及其他几种神经系统疾病的病程。实验研究表明,APOE影响突触形成。我们测定了42例AD患者和160例正常大脑颞上叶皮质中两种突触前蛋白(突触素和 syntaxin 1)以及突触后致密蛋白95(PSD95)的浓度,并确定了APOE基因型。AD患者大脑中两种突触前蛋白的浓度比正常大脑低约三分之二,PSD95的浓度低三分之一。在晚期AD中未发现APOE对突触蛋白有影响。然而,在正常大脑中,ε4与所有三种突触蛋白的较低浓度相关,而ε2与PSD95的显著升高相关(p = 0.03)。对突触蛋白的综合测量显示,从ε2到ε3再到ε4存在显著的线性下降(p = 0.01)。APOE影响正常颞上叶皮质中突触蛋白的浓度,从而可能影响对损伤的反应以及一系列神经系统疾病的风险和预后。

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