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自组装的淀粉样纤维形成 3D 凝胶簇与 2D 片层。

Self-Assembly of Amyloid Fibrils into 3D Gel Clusters versus 2D Sheets.

机构信息

Department of Physics, University of South Florida, Tampa, FL 33620, USA.

出版信息

Biomolecules. 2023 Jan 24;13(2):230. doi: 10.3390/biom13020230.

Abstract

The deposition of dense fibril plaques represents the pathological hallmark for a multitude of human disorders, including many neurodegenerative diseases. Fibril plaques are predominately composed of amyloid fibrils, characterized by their underlying cross beta-sheet architecture. Research into the mechanisms of amyloid formation has mostly focused on characterizing and modeling the growth of individual fibrils and associated oligomers from their monomeric precursors. Much less is known about the mechanisms causing individual fibrils to assemble into ordered fibrillar suprastructures. Elucidating the mechanisms regulating this "secondary" self-assembly into distinct suprastructures is important for understanding how individual protein fibrils form the prominent macroscopic plaques observed in disease. Whether and how amyloid fibrils assemble into either 2D or 3D supramolecular structures also relates to ongoing efforts on using amyloid fibrils as substrates or scaffolds for self-assembling functional biomaterials. Here, we investigated the conditions under which preformed amyloid fibrils of a lysozyme assemble into larger superstructures as a function of charge screening or pH. Fibrils either assembled into three-dimensional gel clusters or two-dimensional fibril sheets. The latter displayed optical birefringence, diagnostic of amyloid plaques. We presume that pH and salt modulate fibril charge repulsion, which allows anisotropic fibril-fibril attraction to emerge and drive the transition from 3D to 2D fibril self-assembly.

摘要

密集纤维斑块的沉积是多种人类疾病的病理标志,包括许多神经退行性疾病。纤维斑块主要由淀粉样纤维组成,其特征是具有潜在的交叉 β-片层结构。对淀粉样形成机制的研究主要集中在描述和模拟单体前体中单个纤维和相关低聚物的生长。关于导致单个纤维组装成有序纤维超结构的机制知之甚少。阐明调节这种“次级”自组装成不同超结构的机制对于理解单个蛋白质纤维如何形成疾病中观察到的明显宏观斑块非常重要。淀粉样纤维是否以及如何组装成 2D 或 3D 超分子结构也与使用淀粉样纤维作为自组装功能生物材料的基质或支架的持续努力有关。在这里,我们研究了溶菌酶的预形成淀粉样纤维在电荷屏蔽或 pH 值的作用下组装成更大超结构的条件。纤维要么组装成三维凝胶簇,要么组装成二维纤维片。后者表现出光学双折射,这是淀粉样斑块的特征。我们推测 pH 值和盐调节纤维的电荷排斥,这允许各向异性纤维-纤维吸引出现,并驱动从 3D 到 2D 纤维自组装的转变。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8a97/9953743/1f3c94d07ba4/biomolecules-13-00230-g001.jpg

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