APL Bioengineering (Jun 2018)

β3-tripeptides act as sticky ends to self-assemble into a bioscaffold

  • Mark P. Del Borgo,
  • Ketav Kulkarni,
  • Mary A. Tonta,
  • Jessie L. Ratcliffe,
  • Rania Seoudi,
  • Adam I. Mechler,
  • Patrick Perlmutter,
  • Helena C. Parkington,
  • Marie-Isabel Aguilar

DOI
https://doi.org/10.1063/1.5020105
Journal volume & issue
Vol. 2, no. 2
pp. 026104 – 026104-9

Abstract

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Peptides comprised entirely of β3-amino acids, commonly referred to as β-foldamers, have been shown to self-assemble into a range of materials. Previously, β-foldamers have been functionalised via various side chain chemistries to introduce function to these materials without perturbation of the self-assembly motif. Here, we show that insertion of both rigid and flexible molecules into the backbone structure of the β-foldamer did not disturb the self-assembly, provided that the molecule is positioned between two β3-tripeptides. These hybrid β3-peptide flanked molecules self-assembled into a range of structures. α-Arginlyglycylaspartic acid (RGD), a commonly used cell attachment motif derived from fibronectin in the extracellular matrix, was incorporated into the peptide sequence in order to form a biomimetic scaffold that would support neuronal cell growth. The RGD-containing sequence formed the desired mesh-like scaffold but did not encourage neuronal growth, possibly due to over-stimulation with RGD. Mixing the RGD peptide with a β-foldamer without the RGD sequence produced a well-defined scaffold that successfully encouraged the growth of neurons and enabled neuronal electrical functionality. These results indicate that β3-tripeptides can form distinct self-assembly units separated by a linker and can form fibrous assemblies. The linkers within the peptide sequence can be composed of a bioactive α-peptide and tuned to provide a biocompatible scaffold.