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阿尔茨海默病中皮质和海马斑块内1型和2型营养不良性神经突的分期相关分布

Stage-correlated distribution of type 1 and 2 dystrophic neurites in cortical and hippocampal plaques in Alzheimer's disease.

作者信息

Thal D R, Härtig W, Schober R

机构信息

Department of Neuropathology, Institute of Pathology, University of Leipzig, Germany.

出版信息

J Hirnforsch. 1998;39(2):175-81.

Abstract

Two types of dystrophic neurites have been described in neuritic plaques in Alzheimer's disease (AD). Type 1 dystrophic neurites display tau-positive paired helical filaments (PHF) while those of type 2 are swollen and positive for both amyloid precursor protein and Chromogranin A. To determine the role of these two types of dystrophic neurites in the development of neuritic plaques, we examined their distribution in CA 1, CA 4, the entorhinal and the temporal cortex throughout all Braak-stages. Fourty cases with AD-related neurofibrillary changes were evaluated semi-quantitatively. The frequency of neuritic plaques displaying both types of dystrophic neurites seemed to increase from stage I to stage IV and to remain stable or slightly decrease in later stages. Staining combinations detecting type 1 (Gallyas, immunohistochemistry against hyperphosphorylated tau-protein) and type 2 dystrophic neurites simultaneously (immunohistochemistry against the amyloid precursor protein or Chromogranin A) showed coexpression of the type 1 and type 2 pattern in single neurites of neuritic plaques. In the entorhinal and temporal cortex, occasional neuritic plaques displayed tau-immunopositive changes in the absence of swollen type 2 neurites. Since amyloid precursor protein is expressed in distal ends of neurites after various brain lesions we suggest that amyloid precursor protein-positive neurites in neuritic plaques indicate dysfunctional axonal transport due to type 1 neurofibrillary changes.

摘要

在阿尔茨海默病(AD)的神经炎性斑块中已描述了两种类型的营养不良性神经突。1型营养不良性神经突显示tau阳性双螺旋丝(PHF),而2型则肿胀,且淀粉样前体蛋白和嗜铬粒蛋白A均呈阳性。为了确定这两种类型的营养不良性神经突在神经炎性斑块形成中的作用,我们检查了它们在所有Braak分期的CA1、CA4、内嗅皮质和颞叶皮质中的分布。对40例伴有AD相关神经原纤维变化的病例进行了半定量评估。显示两种类型营养不良性神经突的神经炎性斑块的频率似乎从I期到IV期增加,在后期保持稳定或略有下降。同时检测1型(Gallyas法、抗高磷酸化tau蛋白免疫组织化学)和2型营养不良性神经突的染色组合(抗淀粉样前体蛋白或嗜铬粒蛋白A免疫组织化学)显示,在神经炎性斑块的单个神经突中1型和2型模式共表达。在内嗅皮质和颞叶皮质中,偶尔有神经炎性斑块在没有肿胀的2型神经突的情况下显示tau免疫阳性变化。由于淀粉样前体蛋白在各种脑损伤后在神经突的远端表达,我们认为神经炎性斑块中淀粉样前体蛋白阳性的神经突表明由于1型神经原纤维变化导致轴突运输功能障碍。

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