TY - JOUR
T1 - Megadalton-sized Dityrosine Aggregates of α-Synuclein Retain High Degrees of Structural Disorder and Internal Dynamics
AU - Verzini, Silvia
AU - Shah, Maliha
AU - Theillet, Francois-Xavier
AU - Belsom, Adam
AU - Bieschke, Jan
AU - Wanker, Erich E.
AU - Rappsilber, Juri
AU - Binolfi, Andres
AU - Selenko, Philipp
N1 - We thank Dr. Rudi Lurz (MPI fuer Molekulare Genetik, Berlin) for help with TEM experiments and Dr. Peter Schmieder and Monika Beerbaum for excellent maintenance of NMR infrastructure. A.B. and J.R. acknowledge support by the Wellcome Trust (103139 and 108504) and the Deutsche Forschungsgemeinschaft (DFG, German Research Foundation, 329673113). The Wellcome Centre for Cell Biology is supported by core funding from the Wellcome Trust (203149). M.S., J.B. and E.E.W. were supported by grant no. 3-12056 from the Helmholtz-Israel Cooperation in Personalized Medicine and grants from the German Research Foundation (SFB618, SFB740, Neurocure), the European Union (EuroSpin and SynSys) and the Helmholtz Association (MSBN and HelMA). S.V. A.B. and P.S. were funded by the European Research Council (ERC) Consolidator Grant NeuroInCellNMR (647474) to P.S. Author contributions - Silvia Verzini: Investigation, Methodology, Visualization, Validation, Writing - original draft. Maliha Shah: Investigation, Validation, Methodology. Francois-Xavier Theillet: Investigation, Validation, Methodology. Adam Belsom: Investigation, Validation, Visualization, Methodology, Resources. Jan Bieschke: Supervision, Methodology, Resources. Erich E. Wanker: Supervision. Juri Rappsilber: Supervision, Resources. Andres Binolfi: Investigation, Validation, Methodology, Visualization, Supervision, Writing - review & editing. Philipp Selenko: Conceptualization, Validation, Writing - review & editing, Project administration, Funding acquisition.
PY - 2020/12/4
Y1 - 2020/12/4
N2 - Heterogeneous aggregates of the human protein α-synuclein (αSyn) are abundantly found in Lewy body inclusions of Parkinson's disease patients. While structural information on classical αSyn amyloid fibrils is available, little is known about the conformational properties of disease-relevant, non-canonical aggregates. Here, we analyze the structural and dynamic properties of megadalton-sized dityrosine adducts of αSyn that form in the presence of reactive oxygen species and cytochrome c, a proapoptotic peroxidase that is released from mitochondria during sustained oxidative stress. In contrast to canonical cross-β amyloids, these aggregates retain high degrees of internal dynamics, which enables their characterization by solution-state NMR spectroscopy. We find that intermolecular dityrosine crosslinks restrict αSyn motions only locally whereas large segments of concatenated molecules remain flexible and disordered. Indistinguishable aggregates form in crowded in vitro solutions and in complex environments of mammalian cell lysates, where relative amounts of free reactive oxygen species, rather than cytochrome c, are rate limiting. We further establish that dityrosine adducts inhibit classical amyloid formation by maintaining αSyn in its monomeric form and that they are non-cytotoxic despite retaining basic membrane-binding properties. Our results suggest that oxidative αSyn aggregation scavenges cytochrome c's activity into the formation of amorphous, high molecular-weight structures that may contribute to the structural diversity of Lewy body deposits.
AB - Heterogeneous aggregates of the human protein α-synuclein (αSyn) are abundantly found in Lewy body inclusions of Parkinson's disease patients. While structural information on classical αSyn amyloid fibrils is available, little is known about the conformational properties of disease-relevant, non-canonical aggregates. Here, we analyze the structural and dynamic properties of megadalton-sized dityrosine adducts of αSyn that form in the presence of reactive oxygen species and cytochrome c, a proapoptotic peroxidase that is released from mitochondria during sustained oxidative stress. In contrast to canonical cross-β amyloids, these aggregates retain high degrees of internal dynamics, which enables their characterization by solution-state NMR spectroscopy. We find that intermolecular dityrosine crosslinks restrict αSyn motions only locally whereas large segments of concatenated molecules remain flexible and disordered. Indistinguishable aggregates form in crowded in vitro solutions and in complex environments of mammalian cell lysates, where relative amounts of free reactive oxygen species, rather than cytochrome c, are rate limiting. We further establish that dityrosine adducts inhibit classical amyloid formation by maintaining αSyn in its monomeric form and that they are non-cytotoxic despite retaining basic membrane-binding properties. Our results suggest that oxidative αSyn aggregation scavenges cytochrome c's activity into the formation of amorphous, high molecular-weight structures that may contribute to the structural diversity of Lewy body deposits.
UR - http://www.scopus.com/inward/record.url?scp=85096610346&partnerID=8YFLogxK
U2 - 10.1016/j.jmb.2020.10.023
DO - 10.1016/j.jmb.2020.10.023
M3 - مقالة
C2 - 33211011
SN - 0022-2836
VL - 432
JO - Journal of Molecular Biology
JF - Journal of Molecular Biology
IS - 24
M1 - 166689
ER -