Racemic Peptides from Amyloid β and Amylin Form Rippled β-Sheets Rather Than Pleated β-Sheets

化学 反平行(数学) 结晶学 胰淀素 测试表 纤维 位阻效应 氢键 结构母题 手性(物理) 立体化学 生物化学 分子 有机化学 小岛 夸克 胰岛素 Nambu–Jona Lasinio模型 内分泌学 物理 磁场 医学 量子力学 手征对称破缺
作者
Amaruka Hazari,M.R. Sawaya,Maria Sajimon,Niko Vlahakis,José A. Rodríguez,David Eisenberg,Jevgenij A. Raskatov
出处
期刊:Journal of the American Chemical Society [American Chemical Society]
卷期号:145 (47): 25917-25926 被引量:5
标识
DOI:10.1021/jacs.3c11712
摘要

The rippled β-sheet was theorized by Pauling and Corey in 1953 as a structural motif in which mirror image peptide strands assemble into hydrogen-bonded periodic arrays with strictly alternating chirality. Structural characterization of the rippled β-sheet was limited to biophysical methods until 2022 when atomic resolution structures of the motif were first obtained. The crystal structural foundation is restricted to four model tripeptides composed exclusively of aromatic residues. Here, we report five new rippled sheet crystal structures derived from amyloid β and amylin, the aggregating toxic peptides of Alzheimer's disease and type II diabetes, respectively. Despite the variation in peptide sequence composition, all five structures form antiparallel rippled β-sheets that extend, like a fibril, along the entire length of the crystalline needle. The long-range packing of the crystals, however, varies. In three of the crystals, the sheets pack face-to-face and exclude water, giving rise to cross-β architectures grossly resembling the steric zipper motif of amyloid fibrils but differing in fundamental details. In the other two crystals, the solvent is encapsulated between the sheets, yielding fibril architectures capable of host–guest chemistry. Our study demonstrates that the formation of rippled β-sheets from aggregating racemic peptide mixtures in three-dimensional (3D) assemblies is a general phenomenon and provides a structural basis for targeting intrinsically disordered proteins.
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