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Multicolor time-stamp reveals the dynamics and toxicity of amyloid deposition

机译:多色时间戳揭示了淀粉样蛋白沉积的动力学和毒性

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摘要

The pathogenic role of amyloid plaques in Alzheimer's disease (AD) remains controversial given poor correlation between plaque burden and cognitive status in clinicopathological studies. However, these postmortem studies cannot provide information about the dynamics of plaque expansion and consequent neurotoxicity. We developed a novel method for plaque birth-dating and growth analysis using sequential labeling with amyloid-binding dyes and postmortem quantitative confocal imaging. Using this technique in an AD mouse model, we find that plaques grow gradually over months with growth slowing in older animals. The degree of neuritic dystrophy correlates with the speed and extent of plaque enlargement suggesting a causal relationship. Surprisingly, new plaques induce a disproportionately large area of neuritic dystrophy whereas with older plaques the degree of injury plateaus despite continued growth. Our results suggest that the kinetics of amyloid deposition is a critical determinant of neurotoxicity, which is completely overlooked by traditional measures of plaque burden.
机译:淀粉样蛋白斑块在阿尔茨海默氏病(AD)中的致病作用仍然存在争议,因为在临床病理研究中,斑块负担与认知状态之间的相关性很差。但是,这些验尸研究无法提供有关斑块扩张和随之而来的神经毒性的动力学信息。我们开发了一种用于斑块出生日期和生长分析的新方法,该方法使用了淀粉样蛋白结合染料和事后定量共聚焦成像的顺序标记。通过在AD小鼠模型中使用该技术,我们发现斑块在数月内逐渐生长,而老年动物的生长速度减慢。神经营养不良的程度与斑块增大的速度和程度相关,表明存在因果关系。出人意料的是,新斑块引起神经营养不良的面积比例过大,而老斑块尽管持续增长,但损伤程度达到稳定水平。我们的结果表明,淀粉样蛋白沉积的动力学是神经毒性的关键决定因素,传统的斑块负荷测量方法完全忽略了这一点。

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