Preparation and Characterization of Stable α-Synuclein Lipoprotein Particles

By Cédric Eichmann, Silvia Campioni, Julia Kowal, Innokentiy Maslennikov, Juan Gerez, Xiaoxia Liu, Joeri Verasdonck, Nadezhda Nespovitaya, Senyon Choe, Beat H. Meier, Paola Picotti, Josep Rizo, Henning Stahlberg, Roland Riek

July 28, 2017

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Title

Preparation and Characterization of Stable α-Synuclein Lipoprotein Particles

Author

Cédric Eichmann, Silvia Campioni, Julia Kowal, Innokentiy Maslennikov, Juan Gerez, Xiaoxia Liu, Joeri Verasdonck, Nadezhda Nespovitaya, Senyon Choe, Beat H. Meier, Paola Picotti, Josep Rizo, Henning Stahlberg, Roland Riek

Year

2016

Journal

The Journal of Biological Chemistry

Abstract

Multiple neurodegenerative diseases are caused by the aggregation of the human α-Synuclein (α-Syn) protein. α-Syn possesses high structural plasticity and the capability of interacting with membranes. Both features are not only essential for its physiological function but also play a role in the aggregation process. Recently it has been proposed that α-Syn is able to form lipid-protein particles reminiscent of high-density lipoproteins. Here, we present a method to obtain a stable and homogeneous population of nanometer-sized particles composed of α-Syn and anionic phospholipids. These particles are called α-Syn lipoprotein (nano)particles to indicate their relationship to high-density lipoproteins formed by human apolipoproteins in vivo and of in vitro self-assembling phospholipid bilayer nanodiscs. Structural investigations of the α-Syn lipoprotein particles by circular dichroism (CD) and magic angle solid-state nuclear magnetic resonance (MAS SS-NMR) spectroscopy establish that α-Syn adopts a helical secondary structure within these particles. Based on cryo-electron microscopy (cryo-EM) and dynamic light scattering (DLS) α-Syn lipoprotein particles have a defined size with a diameter of ∼23 nm. Chemical cross-linking in combination with solution-state NMR and multiangle static light scattering (MALS) of α-Syn particles reveal a high-order protein-lipid entity composed of ∼8–10 α-Syn molecules. The close resemblance in size between cross-linked in vitro-derived α-Syn lipoprotein particles and a cross-linked species of endogenous α-Syn from SH-SY5Y human neuroblastoma cells indicates a potential functional relevance of α-Syn lipoprotein nanoparticles.

Full Article

http://www.jbc.org/content/291/16/8516.short

Instrument

J-815

Keywords

Circular dichroism, Secondary structure, Vesicle interactions, Biochemistry