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Ribbon-like Foldamers for Cellular Uptake and Drug Delivery.

Lubomir L VezenkovVincent MartinNadir BettacheMatthieu SimonAlexandre MesserschmittBaptiste LegrandJean-Louis BantigniesGilles SubraMarie MaynadierVirginie BelletMarcel GarciaJean MartinezMuriel Amblard
Published in: Chembiochem : a European journal of chemical biology (2017)
Different intracellular delivery systems of bioactive compounds have been developed, including cell-penetrating peptides. Although usually nontoxic and biocompatible, these vectors share some of the general drawbacks of peptides, notably low bioavailability and susceptibility to protease degradation, that limit their use. Herein, the conversion of short peptide sequences into poly-α-amino-γ-lactam foldamers that adopt a ribbon-like structure is investigated. This template is used to distribute critical cationic and/or hydrophobic groups on both sides of the backbone, leading to potent short, cell-permeable foldamers with a low positive-charge content. The lead compound showed dramatically improved protease resistance and was able to efficiently deliver a biologically relevant cargo inside cells. This study provided a simple strategy to convert short peptide sequences into efficient protease-resistant cell-penetrating foldamers.
Keyphrases
  • single cell
  • drug delivery
  • cell therapy
  • mesenchymal stem cells
  • ionic liquid
  • oxidative stress
  • cell proliferation
  • mass spectrometry
  • high resolution
  • single molecule
  • gene therapy