Nature Communications (Jan 2024)

Uncovering supramolecular chirality codes for the design of tunable biomaterials

  • Stephen J. Klawa,
  • Michelle Lee,
  • Kyle D. Riker,
  • Tengyue Jian,
  • Qunzhao Wang,
  • Yuan Gao,
  • Margaret L. Daly,
  • Shreeya Bhonge,
  • W. Seth Childers,
  • Tolulope O. Omosun,
  • Anil K. Mehta,
  • David G. Lynn,
  • Ronit Freeman

DOI
https://doi.org/10.1038/s41467-024-45019-2
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 16

Abstract

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Abstract In neurodegenerative diseases, polymorphism and supramolecular assembly of β-sheet amyloids are implicated in many different etiologies and may adopt either a left- or right-handed supramolecular chirality. Yet, the underlying principles of how sequence regulates supramolecular chirality remains unknown. Here, we characterize the sequence specificity of the central core of amyloid-β 42 and design derivatives which enable chirality inversion at biologically relevant temperatures. We further find that C-terminal modifications can tune the energy barrier of a left-to-right chiral inversion. Leveraging this design principle, we demonstrate how temperature-triggered chiral inversion of peptides hosting therapeutic payloads modulates the dosed release of an anticancer drug. These results suggest a generalizable approach for fine-tuning supramolecular chirality that can be applied in developing treatments to regulate amyloid morphology in neurodegeneration as well as in other disease states.