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紫外线诱导的人脑中全长β-淀粉样蛋白沉积物的自发荧光。

UV light-induced autofluorescence of full-length Abeta-protein deposits in the human brain.

作者信息

Thal D R, Ghebremedhin E, Haass C, Schultz C

机构信息

Department of Anatomy, Johann Wolfgang Goethe University, Frankfurt am Main, Germany.

出版信息

Clin Neuropathol. 2002 Jan-Feb;21(1):35-40.

Abstract

The formation of amyloid plaques is a hallmark of Alzheimer's disease (AD). Amyloid plaques and vascular amyloid deposits in cerebral amyloid angiopathy (CAA) consist of the beta-amyloid protein (Abeta) in association with other proteins. These Abeta-deposits can be visualized by thioflavin S, Congo red staining, silver staining methods and immunohistochemistry. Senile plaques also have been shown to exhibit blue autofluorescence. Here we report that UV light-induced autofluorescence is restricted to full-length Abeta-containing amyloid plaques and is also seen in blood vessels affected by CAA. Different types of samples from AD and control cortices were examined: native samples, formalin-fixed paraffin and polyethylene glycol-embedded tissue sections. These samples were viewed with a fluorescence microscope under UV light excitation (360 - 370 nm). By emitting blue fluorescence (>420 nm), amyloid plaques and blood vessels affected by CAA were detected in AD and CAA samples. Combination with immunofluorescence against anti-Abeta1-42, anti-Abeta17-24, and anti-Abeta8-17 demonstrated co-localization of the autofluorescent deposits with full-length Abeta containing Abeta-deposits. N-terminal truncated Abeta-deposits, such as the fleecy amyloid, do not exhibit autofluorescence. In doing so, Abeta-autofluorescence is a suitable method for screening native tissue samples for full-length Abeta-deposits. In contradistinction to conventional and immunohistochemical procedures, detection of plaques and CAA by autofluorescence enables the recognition of full-length Abeta-deposits in the human brain without any chemical interaction whatsoever on the part of Abeta.

摘要

淀粉样斑块的形成是阿尔茨海默病(AD)的一个标志。脑淀粉样血管病(CAA)中的淀粉样斑块和血管淀粉样沉积物由β-淀粉样蛋白(Aβ)与其他蛋白质结合组成。这些Aβ沉积物可以通过硫黄素S、刚果红染色、银染色方法和免疫组织化学进行可视化。老年斑也已被证明会呈现蓝色自发荧光。在此我们报告,紫外线诱导的自发荧光仅限于含有全长Aβ的淀粉样斑块,并且在受CAA影响的血管中也可见。我们检查了来自AD和对照皮质的不同类型样本:天然样本、福尔马林固定石蜡包埋和聚乙二醇包埋的组织切片。这些样本在紫外线激发(360 - 370 nm)下用荧光显微镜观察。通过发出蓝色荧光(>420 nm),在AD和CAA样本中检测到淀粉样斑块和受CAA影响的血管。与抗Aβ1 - 42、抗Aβ17 - 24和抗Aβ8 - 17的免疫荧光相结合,证明了自发荧光沉积物与含有Aβ沉积物的全长Aβ共定位。N端截短的Aβ沉积物,如絮状淀粉样蛋白,不表现出自发荧光。这样一来,Aβ自发荧光是一种筛选天然组织样本中全长Aβ沉积物的合适方法。与传统和免疫组织化学程序不同,通过自发荧光检测斑块和CAA能够在不与Aβ发生任何化学相互作用的情况下识别出人类大脑中的全长Aβ沉积物。

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