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Structural conversion of α-synuclein at the mitochondria induces neuronal toxicity

Output Details

Preprint June 9, 2022

Published August 29, 2022

Aggregation of α-Synuclein (α-Syn) drives Parkinson’s disease, although the initial stages of self-assembly and structural conversion have not been captured inside neurons. We track the intracellular conformational states of α-Syn utilizing a single-molecule FRET biosensor, and show that α-Syn converts from its monomeric state to form two distinct oligomeric states in neurons in a concentration dependent, and sequence specific manner. 3D FRET-CLEM reveals the structural organization, and location of aggregation hotspots inside the cell. Notably multiple intracellular seeding events occur preferentially on membrane surfaces, especially mitochondrial membranes. The mitochondrial lipid, cardiolipin triggers rapid oligomerization of A53T α-Syn, and cardiolipin is sequestered within aggregating lipid-protein complexes. Mitochondrial aggregates impair complex I activity and increase mitochondrial ROS generation, which accelerates the oligomerization of A53T α-Syn, and ultimately causes permeabilization of mitochondrial membranes, and cell death. Patient iPSC derived neurons harboring A53T mutations exhibit accelerated oligomerization that is dependent on mitochondrial ROS, early mitochondrial permeabilization and neuronal death. Our study highlights a mechanism of de novo oligomerization at the mitochondria and its induction of neuronal toxicity.
Tags
  • A53T
  • Membrane
  • Mitochondria
  • Neurons
  • Original Research
  • Parkinson's disease

Meet the Authors

  • Minee Choi, PhD

    Key Personnel: Team Wood

    The Francis Crick Institute

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    Alexandre Chappard

    External Collaborator

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    Bhanu P. Singh

    External Collaborator

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    Catherine Maclachlan

    External Collaborator

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    Margarida Rodrigues

    External Collaborator

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    Evgenia Fedotova

    External Collaborator

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    Alexey V. Berezhnov

    External Collaborator

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    Suman De

    External Collaborator

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    Chris Peddie

    External Collaborator

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    Dilan Athauda

    External Collaborator

  • Gurvir Virdi, MSc

    Key Personnel: Team Wood

    The Francis Crick Institute

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    weijia zhang

    External Collaborator

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    James Evans, MSc

    Key Personnel: Team Wood

    University College London

  • Anna Wernick, BSc

    Key Personnel: Team Hardy Team Wood

    University College London

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    Ziba Shadman Zanjani, MSc

    Key Personnel: Team Wood

    The Francis Crick Institute

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    Plamena R. Angelova

    External Collaborator

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    Noemi Esteras

    External Collaborator

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    Andrey Vinikurov

    External Collaborator

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    Katie Morris

    External Collaborator

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    Kiani Jeacock

    External Collaborator

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    Laura Tosatto

    External Collaborator

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    Daniel Little

    External Collaborator

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    Paul Gissen

    External Collaborator

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    David J. Clarke

    External Collaborator

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    Tilo Kunath

    External Collaborator

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    Lucy Collinson

    External Collaborator

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    David Klenerman

    External Collaborator

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    Andrey Y. Abramov

    External Collaborator

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    Mathew H. Horrocks

    External Collaborator

  • Sonia Gandhi, PhD

    Co-PI (Core Leadership): Team Wood

    University College London

Aligning Science Across Parkinson's
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