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β-折叠多态性的无标记检测

Label-Free Detection of β-Sheet Polymorphism.

作者信息

Weeks William B, Buchanan Lauren E

机构信息

Department of Chemistry, Vanderbilt University, Nashville, Tennessee 37235, United States.

出版信息

J Phys Chem Lett. 2022 Oct 13;13(40):9534-9538. doi: 10.1021/acs.jpclett.2c02292. Epub 2022 Oct 6.

DOI:10.1021/acs.jpclett.2c02292
PMID:36201012
Abstract

The ability to detect and characterize multiple secondary structures or polymorphs within peptide and protein aggregates is crucial to treatment and prevention of amyloidogenic diseases, production of novel biomaterials, and many other applications. Here we report a label-free method to distinguish multiple β-sheet configurations within a single peptide aggregate using two-dimensional infrared spectroscopy. By calculating the transition dipole strength (TDS) spectrum from the ratio of linear and two-dimensional signals, we can extract maximum TDS values which provide higher sensitivity to vibrational coupling, and thus specifics of protein structure, than vibrational frequency alone. TDS spectra of AcKFE8 aggregates reveal two distinct β-sheet structures within fibers that appear homogeneous by other techniques. Furthermore, TDS spectra taken during early stages of aggregation show additional peaks that may indicate the presence of more weakly coupled β-sheet structures. These results demonstrate a unique and powerful spectroscopic method capable of distinguishing multiple oligomeric and polymorphic motifs throughout the aggregation using only native vibrational modes.

摘要

检测和表征肽和蛋白质聚集体中的多种二级结构或多晶型物的能力对于淀粉样变性疾病的治疗和预防、新型生物材料的生产以及许多其他应用至关重要。在此,我们报告一种无标记方法,使用二维红外光谱来区分单个肽聚集体中的多种β-折叠构型。通过从线性信号和二维信号的比率计算跃迁偶极强度(TDS)光谱,我们可以提取最大TDS值,与单独的振动频率相比,该值对振动耦合具有更高的灵敏度,从而能够提供蛋白质结构的细节。AcKFE8聚集体的TDS光谱揭示了纤维内两种不同的β-折叠结构,而其他技术显示这些纤维是均匀的。此外,在聚集早期阶段获得的TDS光谱显示出额外的峰,这可能表明存在耦合较弱的β-折叠结构。这些结果证明了一种独特且强大的光谱方法,该方法仅使用天然振动模式就能在整个聚集过程中区分多种寡聚和多晶型基序。

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