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人 Tau 在脑脂双层膜上的可逆阳离子选择性附着和自组装。

Reversible Cation-Selective Attachment and Self-Assembly of Human Tau on Supported Brain Lipid Membranes.

机构信息

Department of Biosystems Science and Engineering , Eidgenössische Technische Hochschule (ETH) Zurich , Mattenstrasse 26 , 4058 Basel , Switzerland.

Department of Neurology, Alzheimer's Disease Research Laboratory , Harvard Medical School, Massachusetts General Hospital , 114 16th Street , Charlestown , Massachusetts 02129 , United States.

出版信息

Nano Lett. 2018 May 9;18(5):3271-3281. doi: 10.1021/acs.nanolett.8b01085. Epub 2018 Apr 17.

Abstract

Misfolding and aggregation of the neuronal, microtubule-associated protein tau is involved in the pathogenesis of Alzheimer's disease and tauopathies. It has been proposed that neuronal membranes could play a role in tau release, internalization, and aggregation and that tau aggregates could exert toxicity via membrane permeabilization. Whether and how tau interacts with lipid membranes remains a matter of discussion. Here, we characterize the interaction of full-length human tau (htau40) with supported lipid membranes (SLMs) made from brain total lipid extract by time-lapse high-resolution atomic force microscopy (AFM). We observe that tau attaches to brain lipid membranes where it self-assembles in a cation-dependent manner. Sodium triggers the attachment, self-assembly, and growth, whereas potassium inhibits these processes. Moreover, tau assemblies are stable in the presence of sodium and lithium but disassemble in the presence of potassium and rubidium. Whereas the pseudorepeat domains (R1-R4) of htau40 promote the sodium-dependent attachment to the membrane and stabilize the tau assemblies, the N-terminal region promotes tau self-assembly and growth.

摘要

神经元微管相关蛋白 tau 的错误折叠和聚集与阿尔茨海默病和 tau 病的发病机制有关。有人提出,神经元膜可能在 tau 的释放、内化和聚集中发挥作用,tau 聚集物可能通过膜通透性发挥毒性作用。tau 是否以及如何与脂质膜相互作用仍然是一个有争议的问题。在这里,我们通过实时高分辨率原子力显微镜 (AFM) 研究了全长人 tau (htau40) 与脑总脂质提取物制成的支撑脂质膜 (SLM) 的相互作用。我们观察到 tau 附着在脑脂质膜上,并以阳离子依赖性的方式自我组装。钠离子触发附着、自组装和生长,而钾离子抑制这些过程。此外,tau 组装在钠离子和锂存在下稳定,但在钾离子和铷离子存在下解体。尽管 htau40 的假重复结构域 (R1-R4) 促进了钠离子依赖的膜附着并稳定了 tau 组装,但 N 端区域促进了 tau 的自组装和生长。

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