Elevated concentrations cause upright alpha-synuclein conformation at lipid interfaces

Author:

Roeters Steven J.ORCID,Strunge KrisORCID,Pedersen Kasper B.ORCID,Golbek Thaddeus W.,Bregnhøj MikkelORCID,Zhang YugeORCID,Wang Yin,Dong MingdongORCID,Nielsen Janni,Otzen Daniel E.ORCID,Schiøtt BirgitORCID,Weidner TobiasORCID

Abstract

AbstractThe amyloid aggregation of α-synuclein (αS), related to Parkinson’s disease, can be catalyzed by lipid membranes. Despite the importance of lipid surfaces, the 3D-structure and orientation of lipid-bound αS is still not known in detail. Here, we report interface-specific vibrational sum-frequency generation (VSFG) experiments that reveal how monomeric αS binds to an anionic lipid interface over a large range of αS-lipid ratios. To interpret the experimental data, we present a frame-selection method ("ViscaSelect”) in which out-of-equilibrium molecular dynamics simulations are used to generate structural hypotheses that are compared to experimental amide-I spectra via excitonic spectral calculations. At low and physiological αS concentrations, we derive flat-lying helical structures as previously reported. However, at elevated and potentially disease-related concentrations, a transition to interface-protruding αS structures occurs. Such an upright conformation promotes lateral interactions between αS monomers and may explain how lipid membranes catalyze the formation of αS amyloids at elevated protein concentrations.

Funder

Lundbeckfonden

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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