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定量研究β-突触核蛋白和γ-突触核蛋白与模型膜的相互作用。

Quantifying interactions of β-synuclein and γ-synuclein with model membranes.

机构信息

Department of Molecular Biophysics and Biochemistry, Yale University, New Haven, CT 06520-8114, USA.

出版信息

J Mol Biol. 2012 Nov 2;423(4):528-39. doi: 10.1016/j.jmb.2012.08.008. Epub 2012 Aug 23.

Abstract

The synucleins are a family of proteins involved in numerous neurodegenerative pathologies [α-synuclein and β-synuclein (βS)], as well as in various types of cancers [γ-synuclein (γS)]. While the connection between α-synuclein and Parkinson's disease is well established, recent evidence links point mutants of βS to dementia with Lewy bodies. Overexpression of γS has been associated with enhanced metastasis and cancer drug resistance. Despite their prevalence in such a variety of diseases, the native functions of the synucleins remain unclear. They have a lipid-binding motif in their N-terminal region, which suggests interactions with biological membranes in vivo. In this study, we used fluorescence correlation spectroscopy to monitor the binding properties of βS and γS to model membranes and to determine the free energy of the interactions. Our results show that the interactions are most strongly affected by the presence of both anionic lipids and bilayer curvature, while membrane fluidity plays a very minor role. Quantifying the lipid-binding properties of βS and γS provides additional insights into the underlying factors governing the protein-membrane interactions. Such insights not only are relevant to the native functions of these proteins but also highlight their contributions to pathological conditions that are either mediated or characterized by perturbations of these interactions.

摘要

突触核蛋白是一类参与多种神经退行性病理的蛋白质[α-突触核蛋白和β-突触核蛋白(βS)],以及各种类型的癌症[γ-突触核蛋白(γS)]。虽然α-突触核蛋白与帕金森病的联系已经得到充分证实,但最近的证据表明βS 的点突变与路易体痴呆有关。γS 的过表达与增强的转移和癌症药物耐药性有关。尽管它们在如此多种疾病中普遍存在,但突触核蛋白的天然功能仍不清楚。它们在 N 端区域具有脂质结合基序,这表明它们在体内与生物膜相互作用。在这项研究中,我们使用荧光相关光谱法来监测βS 和 γS 与模型膜的结合特性,并确定相互作用的自由能。我们的结果表明,相互作用受阴离子脂质和双层曲率的存在影响最大,而膜流动性的作用很小。定量分析βS 和 γS 的脂质结合特性为控制蛋白质-膜相互作用的基本因素提供了更多的见解。这些见解不仅与这些蛋白质的天然功能有关,而且还突出了它们对由这些相互作用的干扰介导或特征的病理条件的贡献。

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