4.8 Article

Cellular uptake of covalent and non-covalent DNA nanostructures with different sizes and geometries

Journal

NANOSCALE
Volume 11, Issue 22, Pages 10808-10818

Publisher

ROYAL SOC CHEMISTRY
DOI: 10.1039/c9nr02006c

Keywords

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Funding

  1. Progetto di Ateneo, Fun DNA
  2. PRIN (2017) project
  3. FIRC-AIRC fellowship for Italy
  4. Villum Foundation
  5. Danish National Research Foundation
  6. European Union's Horizon 2020 Framework Programme for research and innovation [642023]

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DNA nanostructures with different sizes and shapes, assembled through either covalent or non-covalent bonds, namely tetrahedral and octahedral nanocages, rod-shaped chainmails, square box and rectangular DNA origami structures, were compared for their stability in serum, cell surface binding, internalization efficiency, and intracellular degradation rate. For cell internalization a specific cell system, highly expressing the scavenger receptor LOX-1 was used. The results indicate that LOX-1 binds and internalizes a broad family of DNA structures of different sizes that, however, have a different fate and lifetime inside the cells. Covalently linked tetrahedra, octahedra or chainmails are intact inside cells for up to 18 hours whilst the same DNA nanostructures without covalent bonds along with square box and rectangular origami are rapidly degraded. These data suggest that non-covalently linked structures may be useful for fast drug release whilst the covalently-linked structures could be appropriate vehicles for slow release of molecules.

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