α-Synuclein oligomers form by secondary nucleation

Author:

Xu Catherine K.ORCID,Meisl GeorgORCID,Andrzejewska Ewa A.ORCID,Krainer GeorgORCID,Dear Alexander J.,Castellana-Cruz Marta,Turi Soma,Edu Irina A.ORCID,Vivacqua Giorgio,Jacquat Raphaël P. B.ORCID,Arter William E.,Spillantini Maria Grazia,Vendruscolo MicheleORCID,Linse SaraORCID,Knowles Tuomas P. J.ORCID

Abstract

AbstractOligomeric species arising during the aggregation of α-synuclein are implicated as a major source of toxicity in Parkinson’s disease, and thus a major potential drug target. However, both their mechanism of formation and role in aggregation are largely unresolved. Here we show that, at physiological pH and in the absence of lipid membranes, α-synuclein aggregates form by secondary nucleation, rather than simple primary nucleation, and that this process is enhanced by agitation. Moreover, using a combination of single molecule and bulk level techniques, we identify secondary nucleation on the surfaces of existing fibrils, rather than formation directly from monomers, as the dominant source of oligomers. Our results highlight secondary nucleation as not only the key source of oligomers, but also the main mechanism of aggregate formation, and show that these processes take place under conditions which recapitulate the neutral pH and ionic strength of the cytosol.

Publisher

Springer Science and Business Media LLC

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