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α-突触核蛋白作为一种无规则卷曲的单体——事实还是假象?

α-Synuclein as an intrinsically disordered monomer--fact or artefact?

机构信息

Department of Physical Chemistry, Institute of Chemistry, Federal University of Rio de Janeiro, Brazil.

出版信息

FEBS J. 2013 Oct;280(19):4915-27. doi: 10.1111/febs.12471. Epub 2013 Sep 2.

DOI:10.1111/febs.12471
PMID:23927048
Abstract

Fibrillization of the protein α-synuclein (α-syn) is a hallmark of Parkinson's disease and other α-synucleinopathies. The well-established idea that α-syn is a natively disordered monomer prone to forming fibrils was recently challenged by data showing that the protein mostly exists in vitro and in vivo as helically folded tetramers that are resistant to fibrillization. These apparently conflicting findings may be reconciled by the idea that α-syn exists as a disordered monomer in equilibrium with variable amounts of dynamic oligomeric species. In this context, varying the approaches used for protein purification, such as the method used to lyse cells or the inclusion of denaturing agents, could dramatically perturb this equilibrium and hence alter the relative abundance of the disordered monomer. In the present study, we investigated how the current methods for α-syn purification affect the structure and oligomeric state of the protein, and we discuss the main pitfalls associated with the production of recombinant α-syn in Escherichia coli. We demonstrate that α-syn was expressed in E. coli as a disordered monomer independent of both the cell lysis method and the use of heating/acidification for protein purification. In addition, we provide convincing evidence that the disordered monomer exists in equilibrium with a dynamic dimer, which is not an artefact of the cross-linking protocol as previously suggested. Unlike the helically folded tetramer, α-syn dimer is prone to fibrillate and thus it may be an interesting target for anti-fibrillogenic molecules.

摘要

蛋白质α-突触核蛋白(α-syn)的纤维形成是帕金森病和其他α-突触核蛋白病的标志。最近的数据表明,α-syn 主要以螺旋折叠的四聚体形式存在,不易形成纤维,这一确立的观点挑战了α-syn 是一种天然无序的单体,易于形成纤维的观点,而四聚体对纤维形成具有抗性。这些明显相互矛盾的发现可以通过以下观点来调和,即α-syn 以无序单体的形式存在,与动态寡聚体的可变数量处于平衡状态。在这种情况下,改变蛋白质纯化方法,如用于裂解细胞的方法或加入变性剂,可能会极大地破坏这种平衡,从而改变无序单体的相对丰度。在本研究中,我们研究了当前用于α-syn 纯化的方法如何影响蛋白质的结构和寡聚状态,并讨论了与在大肠杆菌中生产重组α-syn 相关的主要陷阱。我们证明,α-syn 在大肠杆菌中以无序单体的形式表达,这与细胞裂解方法和用于蛋白质纯化的加热/酸化无关。此外,我们提供了令人信服的证据表明,无序单体与动态二聚体处于平衡状态,这与以前提出的交联方案无关,而不是二聚体的假象。与螺旋折叠的四聚体不同,α-syn 二聚体易于形成纤维,因此它可能是抗纤维形成分子的一个有趣靶点。

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