AI Article Synopsis

  • Amyloid-like assembly can create new nanomaterials with special features, beyond its link to diseases.
  • Using Fmoc diphenylalanine peptide, researchers found that histidine influences its assembly and promotes enzyme-like activity that generates reactive oxygen species (ROS).
  • This effect is also seen in Aβ filaments, which are linked to neuron damage and Alzheimer's, indicating that histidine could play a key role in both nanomaterial design and understanding disease mechanisms.

Article Abstract

Amyloid-like assembly is not only associated with pathological events, but also leads to the development of novel nanomaterials with unique properties. Herein, using Fmoc diphenylalanine peptide (Fmoc-F-F) as a minimalistic model, we found that histidine can modulate the assembly behavior of Fmoc-F-F and induce enzyme-like catalysis. Specifically, the presence of histidine rearranges the β structure of Fmoc-F-F to assemble nanofilaments, resulting in the formation of active site to mimic peroxidase-like activity that catalyzes ROS generation. A similar catalytic property is also observed in Aβ assembled filaments, which is correlated with the spatial proximity between intermolecular histidine and F-F. Notably, the assembled Aβ filaments are able to induce cellular ROS elevation and damage neuron cells, providing an insight into the pathological relationship between Aβ aggregation and Alzheimer's disease. These findings highlight the potential of histidine as a modulator in amyloid-like assembly of peptide nanomaterials exerting enzyme-like catalysis.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10509148PMC
http://dx.doi.org/10.1038/s41467-023-41591-1DOI Listing

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