Origin of Secondary Structure Transitions and Peptide Self-Assembly Propensity in Trifluoroethanol–Water Mixtures

圆二色性 化学 蛋白质二级结构 测试表 两亲性 盐(化学) 水溶液 生物物理学 结晶学 纤维 自组装 淀粉样蛋白(真菌学) 立体化学 生物化学 有机化学 无机化学 聚合物 共聚物 生物
作者
Anup Kumar Prasad,Rajarshi Samajdar,Ajay S. Panwar,Lisandra L. Martin
出处
期刊:Journal of Physical Chemistry B [American Chemical Society]
卷期号:128 (32): 7736-7749
标识
DOI:10.1021/acs.jpcb.4c02594
摘要

Membrane-peptide interactions are key to the formation of helical intermediates in the early stages of amyloidogenesis. Aqueous solutions of 2,2,2-trifluoroethanol (TFE) provide a membrane-mimetic environment capable of promoting and stabilizing local peptide interactions. Uperin 3.5 (U3.5), a 17-residue and amidated antimicrobial peptide, is unstructured in water but self-assembles into fibrils in the presence of salt. Secondary structure transitions linked to U3.5 self-assembly were investigated in TFE/water mixtures, in both the absence and presence of salt, to assess the role of membrane-peptide interactions on peptide self-assembly and amyloid formation. A 5-to-7-fold increase in fibril yield of U3.5 was observed at low TFE concentrations (10% TFE/water v/v) compared with physiological buffer but only in the presence of salt. No aggregation was observed in salt-free TFE/water mixtures. Circular dichroism spectra showed that partial helical structures, initially stabilized by TFE, transitioned to β-sheet-rich aggregates in a saline buffer. Molecular dynamics simulations confirmed that TFE and salt act synergistically to enhance peptide-peptide interactions, resulting in β-sheet-rich U3.5 oligomers at low TFE concentrations. Specifically, TFE stabilized amphipathic, helical intermediates, leading to increased peptide-peptide attraction through hydrophobic interactions. The presence of salt further enhanced the peptide-peptide interactions by screening positively charged residues. Thus, the study revealed the role of a membrane mimic in stabilizing helical intermediates on the pathway to amyloid formation in the antimicrobial U3.5 peptide.

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