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寡聚β-淀粉样蛋白1-42的制备及对海马切片突触可塑性损伤的诱导

Preparation of oligomeric beta-amyloid 1-42 and induction of synaptic plasticity impairment on hippocampal slices.

作者信息

Fa Mauro, Orozco Ian J, Francis Yitshak I, Saeed Faisal, Gong Yimin, Arancio Ottavio

机构信息

Taub Institute for Research on Alzheimer's Disease and Aging Brain, Columbia University, NY, USA.

出版信息

J Vis Exp. 2010 Jul 14(41):1884. doi: 10.3791/1884.

DOI:10.3791/1884
PMID:20644518
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3156071/
Abstract

Impairment of synaptic connections is likely to underlie the subtle amnesic changes occurring at the early stages of Alzheimer s Disease (AD). beta-amyloid (A beta), a peptide produced in high amounts in AD, is known to reduce Long-Term Potentiation (LTP), a cellular correlate of learning and memory. Indeed, LTP impairment caused by A beta is a useful experimental paradigm for studying synaptic dysfunctions in AD models and for screening drugs capable of mitigating or reverting such synaptic impairments. Studies have shown that A beta produces the LTP disruption preferentially via its oligomeric form. Here we provide a detailed protocol for impairing LTP by perfusion of oligomerized synthetic A beta1-42 peptide onto acute hippocampal slices. In this video, we outline a step-by-step procedure for the preparation of oligomeric A beta(1-42;). Then, we follow an individual experiment in which LTP is reduced in hippocampal slices exposed to oligomerized A beta(1-42;) compared to slices in a control experiment where no A beta(1-42;) exposure had occurred.

摘要

突触连接受损可能是阿尔茨海默病(AD)早期出现细微失忆变化的基础。β-淀粉样蛋白(Aβ)是AD中大量产生的一种肽,已知它会降低长时程增强(LTP),而LTP是学习和记忆的细胞相关指标。事实上,由Aβ引起的LTP损伤是研究AD模型中突触功能障碍以及筛选能够减轻或逆转这种突触损伤的药物的有用实验范式。研究表明,Aβ优先通过其寡聚体形式导致LTP破坏。在这里,我们提供了一个详细的方案,通过将寡聚化的合成Aβ1-42肽灌注到急性海马切片上来损伤LTP。在本视频中,我们概述了制备寡聚体Aβ(1-42)的分步程序。然后,我们展示了一个单独的实验,与未暴露于Aβ(1-42)的对照实验中的切片相比,暴露于寡聚化Aβ(1-42)的海马切片中的LTP降低。