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特定疾病的 tau 纤维通过多态中间产物组装。

Disease-specific tau filaments assemble via polymorphic intermediates.

机构信息

MRC Laboratory of Molecular Biology, Cambridge, UK.

Thermo Fisher Scientific, Eindhoven, The Netherlands.

出版信息

Nature. 2024 Jan;625(7993):119-125. doi: 10.1038/s41586-023-06788-w. Epub 2023 Nov 29.

Abstract

Intermediate species in the assembly of amyloid filaments are believed to play a central role in neurodegenerative diseases and may constitute important targets for therapeutic intervention. However, structural information about intermediate species has been scarce and the molecular mechanisms by which amyloids assemble remain largely unknown. Here we use time-resolved cryogenic electron microscopy to study the in vitro assembly of recombinant truncated tau (amino acid residues 297-391) into paired helical filaments of Alzheimer's disease or into filaments of chronic traumatic encephalopathy. We report the formation of a shared first intermediate amyloid filament, with an ordered core comprising residues 302-316. Nuclear magnetic resonance indicates that the same residues adopt rigid, β-strand-like conformations in monomeric tau. At later time points, the first intermediate amyloid disappears and we observe many different intermediate amyloid filaments, with structures that depend on the reaction conditions. At the end of both assembly reactions, most intermediate amyloids disappear and filaments with the same ordered cores as those from human brains remain. Our results provide structural insights into the processes of primary and secondary nucleation of amyloid assembly, with implications for the design of new therapies.

摘要

中间物种在淀粉样纤维的组装中被认为起着核心作用,可能是治疗干预的重要靶点。然而,关于中间物种的结构信息一直很少,淀粉样纤维组装的分子机制在很大程度上仍然未知。在这里,我们使用时间分辨低温电子显微镜研究重组截断的 tau(氨基酸残基 297-391)在体外组装成阿尔茨海默病的双螺旋纤维或慢性创伤性脑病的纤维。我们报告了共享的第一个中间淀粉样纤维的形成,其有序核心由残基 302-316 组成。核磁共振表明,相同的残基在单体 tau 中采用刚性的β-折叠构象。在稍后的时间点,第一个中间淀粉样纤维消失,我们观察到许多不同的中间淀粉样纤维,其结构取决于反应条件。在两个组装反应的末端,大多数中间淀粉样纤维消失,并且与来自人脑的纤维具有相同有序核心的纤维仍然存在。我们的结果为淀粉样纤维组装的初级和次级成核过程提供了结构见解,对新疗法的设计具有启示意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/482f/10764278/1fd0c6d84810/41586_2023_6788_Fig1_HTML.jpg

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