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Designed peptides as nanomolar cross-amyloid inhibitors acting via supramolecular nanofiber co-assembly

Medicine and Health

Designed peptides as nanomolar cross-amyloid inhibitors acting via supramolecular nanofiber co-assembly

K. Taş, B. D. Volta, et al.

This groundbreaking research unveils how constrained peptides, designed to mimic the amyloid-β peptide, act as powerful nanomolar cross-amyloid inhibitors. Conducted by a team including Karin Taş and Beatrice Dalla Volta, the study reveals these peptides effectively suppress cross-seeding of toxic amyloids, pointing towards promising anti-amyloid drug options and novel nanomaterials.

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Abstract
Amyloid self-assembly is linked to numerous devastating cell-degenerative diseases. However, designing inhibitors of this pathogenic process remains a major challenge. Cross-interactions between amyloid-β peptide (Aβ) and islet amyloid polypeptide (IAPP), key polypeptides of Alzheimer's disease (AD) and type 2 diabetes (T2D), have been suggested to link AD with T2D pathogenesis. Here, we show that constrained peptides designed to mimic the Aβ amyloid core (ACMs) are nanomolar cross-amyloid inhibitors of both IAPP and Aβ42 and effectively suppress reciprocal cross-seeding. Remarkably, ACMs act by co-assembling with IAPP or Aβ42 into amyloid fibril-resembling but non-toxic nanofibers and their highly ordered superstructures. Co-assembled nanofibers exhibit various potentially beneficial features including thermolability, proteolytic degradability, and effective cellular clearance which are reminiscent of labile/reversible functional amyloids. ACMs are thus promising leads for potent anti-amyloid drugs in both T2D and AD while the supramolecular nanofiber co-assemblies should inform the design of novel functional (hetero-)amyloid-based nanomaterials for biomedical/biotechnological applications.
Publisher
Nature Communications
Published On
Aug 25, 2022
Authors
Karin Taş, Beatrice Dalla Volta, Christina Lindner, Omar El Bounkari, Kathleen Hille, Yuan Tian, Xènia Puig-Bosch, Markus Ballmann, Simon Hornung, Martin Ortner, Sophia Prem, Laura Meier, Gerhard Rammes, Martin Haslbeck, Christian Weber, Remco T. A. Megens, Jürgen Bernhagen, Aphrodite Kapurniotu
Tags
amyloid self-assembly
peptides
cross-amyloid inhibitors
non-toxic nanofibers
co-assembly
drug leads
nanomaterials
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