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Porous Silicon and Polymer Nanocomposites for Delivery of Peptide Nucleic Acids as Anti-MicroRNA Therapies.

Kelsey R Beavers, Thomas A Werfel, Tianwei Shen, Taylor E Kavanaugh, Kameron V Kilchrist, Jeremy W Mares, Joshua S Fain, Carrie B Wiese, Kasey C Vickers, Sharon M Weiss, Craig L Duvall
Advanced Materials 2016 September
Self-assembled polymer/porous silicon nanocomposites overcome intracellular and systemic barriers for in vivo application of peptide nucleic acid (PNA) anti-microRNA therapeutics. Porous silicon (PSi) is leveraged as a biodegradable scaffold with high drug-cargo-loading capacity. Functionalization with a diblock polymer improves PSi nanoparticle colloidal stability, in vivo pharmacokinetics, and intracellular bioavailability through endosomal escape, enabling PNA to inhibit miR-122 in vivo.

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