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球状淀粉样β肽寡聚体——阿尔茨海默病中一种同质且稳定的神经病理学蛋白。

Globular amyloid beta-peptide oligomer - a homogenous and stable neuropathological protein in Alzheimer's disease.

作者信息

Barghorn Stefan, Nimmrich Volker, Striebinger Andreas, Krantz Carsten, Keller Patrick, Janson Bodo, Bahr Michael, Schmidt Martin, Bitner Robert S, Harlan John, Barlow Eve, Ebert Ulrich, Hillen Heinz

机构信息

Neuroscience Discovery Research, Abbott GmbH and Co. KG, Ludwigshafen, Germany.

出版信息

J Neurochem. 2005 Nov;95(3):834-47. doi: 10.1111/j.1471-4159.2005.03407.x. Epub 2005 Aug 31.

DOI:10.1111/j.1471-4159.2005.03407.x
PMID:16135089
Abstract

Amyloid beta-peptide (Abeta)(1-42) oligomers have recently been discussed as intermediate toxic species in Alzheimer's disease (AD) pathology. Here we describe a new and highly stable Abeta(1-42) oligomer species which can easily be prepared in vitro and is present in the brains of patients with AD and Abeta(1-42)-overproducing transgenic mice. Physicochemical characterization reveals a pure, highly water-soluble globular 60-kDa oligomer which we named 'Abeta(1-42) globulomer'. Our data indicate that Abeta(1-42) globulomer is a persistent structural entity formed independently of the fibrillar aggregation pathway. It is a potent antigen in mice and rabbits eliciting generation of Abeta(1-42) globulomer-specific antibodies that do not cross-react with amyloid precursor protein, Abeta(1-40) and Abeta(1-42) monomers and Abeta fibrils. Abeta(1-42) globulomer binds specifically to dendritic processes of neurons but not glia in hippocampal cell cultures and completely blocks long-term potentiation in rat hippocampal slices. Our data suggest that Abeta(1-42) globulomer represents a basic pathogenic structural principle also present to a minor extent in previously described oligomer preparations and that its formation is an early pathological event in AD. Selective neutralization of the Abeta globulomer structure epitope is expected to have a high potential for treatment of AD.

摘要

β-淀粉样肽(Aβ)(1-42)寡聚体最近被认为是阿尔茨海默病(AD)病理过程中的中间毒性物质。在此,我们描述了一种新的、高度稳定的Aβ(1-42)寡聚体,它可以在体外轻松制备,并且存在于AD患者和过度表达Aβ(1-42)的转基因小鼠的大脑中。物理化学特征显示这是一种纯的、高度水溶性的球状60 kDa寡聚体,我们将其命名为“Aβ(1-42)球聚体”。我们的数据表明,Aβ(1-42)球聚体是一种独立于纤维状聚集途径形成的持久结构实体。它是小鼠和兔子体内的一种强效抗原,能引发产生不与淀粉样前体蛋白、Aβ(1-40)和Aβ(1-42)单体以及Aβ纤维发生交叉反应的Aβ(1-42)球聚体特异性抗体。在海马细胞培养物中,Aβ(1-42)球聚体特异性结合神经元的树突状突起而非胶质细胞,并完全阻断大鼠海马切片中的长时程增强。我们的数据表明,Aβ(1-42)球聚体代表了一种基本的致病结构原理,在先前描述的寡聚体制剂中也有少量存在,并且其形成是AD早期的病理事件。选择性中和Aβ球聚体结构表位有望具有治疗AD的巨大潜力。

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