Self-limiting multimerization of α-synuclein on membrane and its implication in Parkinson’s diseases.

Self-limiting multimerization of α-synuclein on membrane and its implication in Parkinson’s diseases.

Publication date: Oct 11, 2024

α-Synuclein (α-syn), a crucial molecule in Parkinson’s disease (PD), is known for its interaction with lipid membranes, which facilitates vesicle trafficking and modulates its pathological aggregation. Deciphering the complexity of the membrane-binding behavior of α-syn is crucial to understand its functions and the pathology of PD. Here, we used single-molecule imaging to show that α-syn forms multimers on lipid membranes with huge intermultimer distances. The multimers are characterized by self-limiting growth, manifesting in concentration-dependent exchanges of monomers, which are fast at micromolar concentrations and almost stop at nanomolar concentrations. We further uncovered movement patterns of α-syn’s occasional trapping on membranes, which may be attributed to sparse lipid packing defects. Mutations such as E46K and E35K may disrupt the limit on the growth, resulting in larger multimers and accelerated amyloid fibril formation. This work emphasizes sophisticated regulation of α-syn multimerization on membranes as a critical underlying factor in the PD pathology.

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Concepts Keywords
Amyloid alpha-Synuclein
Fast alpha-Synuclein
Parkinson Amyloid
Pathology Amyloid
Trafficking Cell Membrane
Humans
Mutation
Parkinson Disease
Protein Multimerization
Single Molecule Imaging

Semantics

Type Source Name
disease MESH Parkinson’s disease
disease MESH defects
pathway KEGG Parkinson disease

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