2025-10-01 バース大学
<関連情報>
- https://www.bath.ac.uk/announcements/bath-scientists-design-peptide-switch-that-keeps-parkinsons-protein-in-its-healthy-form/
- https://pubs.acs.org/doi/10.1021/jacsau.5c00694
Stabilizing a Native Fold of Alpha-Synuclein with Short Helix-Constrained Peptides
Richard M. Meade,Scott G. Allen,Amy J. Lopez,Christopher Williams,Iona Thomas-Wright,Rachel Heon-Roberts,Mara Carey-Wood,T. M. Simon Tang,Julia E. Sero,Vicky L. Hunt,Richard Wade-Martins,Matthew P. Crump,and Jody M. Mason
JACS Au Published: September 4, 2025
DOI:https://doi.org/10.1021/jacsau.5c00694
Abstract
Preventing the aggregation of α-synuclein (αS) into toxic oligomers and conformers is a major therapeutic goal in conditions such as Parkinson’s disease and Lewy body dementia. However, the large intracellular protein–protein interfaces within such aggregates make this a challenging target for small molecule approaches or biologics, which often lack cell permeability. Peptides occupy a suitable middle ground and are increasingly being explored as preventative treatments. We previously showed that the N-terminal lipid binding region (αS1–25) inhibits αS aggregation. Building on this, we designed a series of N- and C-terminal truncations to systematically reduce the peptide length, enabling a 56% downsizing (i.e., truncating 92% of the full-length αS protein), to identify the smallest functional unit capable of binding αS and potently blocking its aggregation and toxicity. We next introduced seven systematic i → i + 4 helix constraints to assess impact on (i) α-helicity, (ii) aggregation inhibition, (iii) serum stability, (iv) neuronal uptake, and (v) phenotypic rescue. This work maps key amphipathic features and identifies residues that are critical for αS engagement and inhibitory activity. The most effective helix-constrained peptide, αS2–12(L6), showed marked improvements across all metrics and represents a strong candidate for further therapeutic development.
