KTKEGV repeat motifs are key mediators of normal α-synuclein tetramerization: Their mutation causes excess monomers and neurotoxicity

KTKEGV repeat motifs are key mediators of normal α-synuclein tetramerization: Their mutation causes excess monomers and neurotoxicity

α-Synuclein (αS) is a highly abundant neuronal protein that aggregates into β-sheet–rich inclusions in Parkinson’s disease (PD). αS was long thought to occur as a natively unfolded monomer, but recent work suggests it also occurs normally in α-helix–rich tetramers and related multimers. To elucidate...

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Veröffentlicht in:Proceedings of the National Academy of Sciences - PNAS 2015-08, Vol.112 (31), p.9596-9601
Hauptverfasser: Dettmer, Ulf, Newman, Andrew J., von Saucken, Victoria E., Bartels, Tim, Selkoe, Dennis
Format: Artikel
Sprache:eng
Schlagworte:
alpha-Synuclein - chemistry
alpha-Synuclein - genetics
alpha-Synuclein - toxicity
Amino Acid Motifs
Amino Acid Sequence
Animals
Biological Sciences
Cell Death - drug effects
Conserved Sequence
Cross-Linking Reagents - pharmacology
Humans
Inclusion Bodies - drug effects
Inclusion Bodies - metabolism
Microscopy, Fluorescence
Molecular Sequence Data
Mutant Proteins - metabolism
Mutation - genetics
Neurons - drug effects
Neurons - metabolism
Neurons - pathology
Protein Multimerization
Rats, Sprague-Dawley
Repetitive Sequences, Amino Acid
Sequence Deletion
Structure-Activity Relationship
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Zusammenfassung:α-Synuclein (αS) is a highly abundant neuronal protein that aggregates into β-sheet–rich inclusions in Parkinson’s disease (PD). αS was long thought to occur as a natively unfolded monomer, but recent work suggests it also occurs normally in α-helix–rich tetramers and related multimers. To elucidate the fundamental relationship between αS multimers and monomers in living neurons, we performed systematic mutagenesis to abolish self-interactions and learn which structural determinants underlie native multimerization. Unexpectedly, tetramers/multimers still formed in cells expressing each of 14 sequential 10-residue deletions across the 140-residue polypeptide. We postulated compensatory effects among the six highly conserved and one to three additional αS repeat motifs (consensus: KTKEGV), consistent with αS and its homologs β- andγ-synuclein all forming tetramers while sharing only the repeats. Upon inserting in-register missense mutations into six or more αS repeats, certain mutations abolished tetramer formation, shown by intact-cell cross-linking and independently by fluorescent-protein complementation. For example, altered repeat motifs KLKEGV, KTKKGV, KTKEIV, or KTKEGW did not support tetramerization, indicating the importance of charged or small residues. When we expressed numerous different in-register repeat mutants in human neural cells, all multimer-abolishing but no multimer-neutral mutants caused frank neurotoxicity akin to the proapoptotic protein Bax. The multimer-abolishing variants became enriched in buffer-insoluble cell fractions and formed round cytoplasmic inclusions in primary cortical neurons. We conclude that the αS repeat motifs mediate physiological tetramerization, and perturbing them causes PD-like neurotoxicity. Moreover, the mutants we describe are valuable tools for studying normal and pathological properties of αS and screening for tetramer-stabilizing therapeutics.
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.1505953112