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Intrinsically disordered proteins in the neurodegenerative processes: formation of tau protein paired helical filaments and their analysis.

机译:神经退行性过程中的内在无序蛋白:tau蛋白配对螺旋丝的形成及其分析。

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摘要

1. Several intrinsically disordered proteins (IDPs) play principal role in the neurodegenerative processes of various types. Among them, alpha-synuclein is involved in Parkinson's disease, prion protein in transmissible spongiform encephalopathies, and tau protein in Alzheimer's disease (AD) and related tauopathies. Neuronal damage in AD is accompanied by the presence of tau protein fibrils composed of paired helical filaments (PHF). 2. Tau protein represents a typical IDP. IDPs do not exhibit any stable secondary structure in the free form, but they are able to fold after binding to targets and contain regions with large propensity to adopt a defined type of secondary structure. Binding-folding event at tau protein leading to PHF generation is believed to happen in the course of tauopathies. 3. Detailed molecular topology of PHF formation is unknown. There are evidences about the cross-beta structure in PHF core; however the precise arrangement of the tau polypeptide chain is unclear. In this review we summarize current attempts at in vitro PHF reconstruction and the development of methods for PHF structure determination. The emphasis is put on the monoclonal antibodies used as structural molecular probes for research on the role of IDPs in pathogenesis of neurodegenerative diseases.
机译:1.几种内在失调的蛋白质(IDP)在各种类型的神经变性过程中起主要作用。其中,α-突触核蛋白与帕金森氏病有关,在传染性海绵状脑病中与in病毒蛋白有关,在阿尔茨海默氏病(AD)和相关的疾病中与tau蛋白有关。 AD中的神经元损伤伴随着由成对的螺旋丝(PHF)组成的tau蛋白原纤维的存在。 2. Tau蛋白代表典型的IDP。 IDP没有以游离形式显示任何稳定的二级结构,但是它们能够在与靶标结合后折叠,并包含倾向于采用确定类型的二级结构的区域。据信tau蛋白在tau蛋白上的结合折叠事件发生在tauopathies的过程中。 3. PHF形成的详细分子拓扑是未知的。有证据表明在PHF核心中有交叉β结构。然而,tau多肽链的精确排列尚不清楚。在这篇综述中,我们总结了目前在体外PHF重建中的尝试以及PHF结构确定方法的发展。重点放在用作结构分子探针的单克隆抗体上,以研究IDP在神经退行性疾病发病机理中的作用。

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