α-synuclein oligomers interact with ATP synthase and open the permeability transition pore in Parkinson’s disease

Marthe H. R. Ludtmann(Royal Veterinary College), Plamena R. Angelova(University College London), Mathew H. Horrocks(University of Cambridge), Minee L. Choi(The Francis Crick Institute), Margarida Rodrigues(University of Cambridge), Artyom Y. Baev, Alexey V. Berezhnov(Institute of Cell Biophysics), Zhi Yao(The Francis Crick Institute), Daniel Little(MRC Laboratory for Molecular Cell Biology), Blerida Banushi(MRC Laboratory for Molecular Cell Biology), Afnan Saleh Al‐Menhali(Anti-Doping Laboratory), Rohan T. Ranasinghe(University of Cambridge), Daniel R. Whiten(University of Cambridge), Ratsuda Yapom(MRC Centre for Regenerative Medicine), Karamjit Singh Dolt(MRC Centre for Regenerative Medicine), Michael J. Devine(MRC Laboratory for Molecular Cell Biology), Paul Gissen(MRC Laboratory for Molecular Cell Biology), Tilo Kunath(MRC Centre for Regenerative Medicine), Morana Jaganjac(Anti-Doping Laboratory), Evgeny V. Pavlov(New York University), David Klenerman(University of Cambridge), Andrey Y. Abramov(Institute of Structural and Molecular Biology), Sonia Gandhi(Sobell House)
Nature Communications
June 6, 2018
10.1038/s41467-018-04422-2
Cited by 501Open Access
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Abstract

Protein aggregation causes α-synuclein to switch from its physiological role to a pathological toxic gain of function. Under physiological conditions, monomeric α-synuclein improves ATP synthase efficiency. Here, we report that aggregation of monomers generates beta sheet-rich oligomers that localise to the mitochondria in close proximity to several mitochondrial proteins including ATP synthase. Oligomeric α-synuclein impairs complex I-dependent respiration. Oligomers induce selective oxidation of the ATP synthase beta subunit and mitochondrial lipid peroxidation. These oxidation events increase the probability of permeability transition pore (PTP) opening, triggering mitochondrial swelling, and ultimately cell death. Notably, inhibition of oligomer-induced oxidation prevents the pathological induction of PTP. Inducible pluripotent stem cells (iPSC)-derived neurons bearing SNCA triplication, generate α-synuclein aggregates that interact with the ATP synthase and induce PTP opening, leading to neuronal death. This study shows how the transition of α-synuclein from its monomeric to oligomeric structure alters its functional consequences in Parkinson's disease.

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