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阿尔茨海默病的神经病理学

Neuropathology of Alzheimer's disease.

作者信息

Perl Daniel P

机构信息

Neuropathology Division, Mount Sinai School of Medicine, New York, NY, USA.

出版信息

Mt Sinai J Med. 2010 Jan-Feb;77(1):32-42. doi: 10.1002/msj.20157.

Abstract

Alois Alzheimer first pointed out that the disease which would later bear his name has a distinct and recognizable neuropathological substrate. Since then, much has been added to our understanding of the pathological lesions associated with the condition. The 2 primary cardinal lesions associated with Alzheimer's disease are the neurofibrillary tangle and the senile plaque. The neurofibrillary tangle consists of abnormal accumulations of abnormally phosphorylated tau within the perikaryal cytoplasm of certain neurons. The senile plaque consists of a central core of beta-amyloid, a 4-kD peptide, surrounded by abnormally configured neuronal processes or neurites. Other neuropathological lesions are encountered in cases of Alzheimer's disease, but the disease is defined and recognized by these 2 cardinal lesions. Other lesions include poorly understood changes such as granulovacuolar degeneration and eosinophilic rodlike bodies (Hirano bodies). The loss of synaptic components is a change that clearly has a significant impact on cognitive function and represents another important morphological alteration. It is important to recognize that distinguishing between Alzheimer's disease, especially in its early stages, and normal aging may be very difficult, particularly if one is examining the brains of patients who died at an advanced old age. It is also noted that instances of pure forms of Alzheimer's disease, in the absence of other coexistent brain disease processes, such as infarctions or Parkinson's disease-related lesions, are relatively uncommon, and this must be taken into account by researchers who employ postmortem brain tissues for research.

摘要

阿洛伊斯·阿尔茨海默首先指出,这种后来以他的名字命名的疾病具有独特且可识别的神经病理学基础。从那时起,我们对与该病症相关的病理病变的理解有了很多补充。与阿尔茨海默病相关的2种主要基本病变是神经原纤维缠结和老年斑。神经原纤维缠结由某些神经元胞浆内异常磷酸化的tau蛋白异常聚集而成。老年斑由β淀粉样蛋白(一种4-kD肽)的中央核心组成,周围是异常构型的神经元突起或神经突。在阿尔茨海默病病例中还会遇到其他神经病理学病变,但该疾病是由这2种基本病变来定义和识别的。其他病变包括如颗粒空泡变性和嗜酸性棒状体( Hirano小体)等了解甚少的变化。突触成分的丧失是一种明显对认知功能有重大影响的变化,代表了另一种重要的形态学改变。重要的是要认识到,区分阿尔茨海默病,尤其是在其早期阶段,与正常衰老可能非常困难,特别是如果检查的是高龄死亡患者的大脑。还应注意的是,在没有其他并存的脑部疾病过程(如梗死或帕金森病相关病变)的情况下,纯形式的阿尔茨海默病相对少见,使用死后脑组织进行研究的研究人员必须考虑到这一点。

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