| Literature DB >> 27214742 |
Giulia Vindigni1, Sofia Raniolo1, Alessio Ottaviani2, Mattia Falconi2, Oskar Franch, Birgitta R Knudsen, Alessandro Desideri2, Silvia Biocca1.
Abstract
DNA offers excellent programming properties for the generation of nanometer-scaled polyhedral structures with a broad variety of potential applications. Translation to biomedical applications requires improving stability in biological fluids, efficient and selective cell binding, and/or internalization of the assembled DNA nanostructures. Here, we report an investigation on the selective mechanism of cellular uptake of pristine DNA nanocages in cells expressing the receptor "oxidized low-density lipoprotein receptor-1" (LOX-1), a scavenger receptor associated with cardiovascular diseases and, more recently, identified as a tumor marker. For this purpose a truncated octahedral DNA nanocage functionalized with a single biotin molecule, which allows DNA cage detection through the biotin-streptavidin assays, was constructed. The results indicate that DNA nanocages are stable in biological fluids, including human serum, and are selectively bound and very efficiently internalized in vesicles only in LOX-1-expressing cells. The amount of internalized cages is 30 times higher in LOX-1-expressing cells than in normal fibroblasts, indicating that the receptor-mediated uptake of pristine DNA nanocages can be pursued for a selective cellular internalization. These results open the route for a therapeutic use of pristine DNA cages targeting LOX-1-overexpressing tumor cells.Entities:
Keywords: DNA nanocage stability; DNA nanotechnology; LOX-1; cell uptake; drug delivery; scavenger receptors
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Year: 2016 PMID: 27214742 DOI: 10.1021/acsnano.6b01402
Source DB: PubMed Journal: ACS Nano ISSN: 1936-0851 Impact factor: 15.881