2017 Annual Meeting
(17b) Targeted Polyanhydride Nanoparticles to Combat Neurodegeneration
Authors
Targeted nano-carriers can improve the local bioavailability of therapeutics by targeting these hurdles and providing sustained release. Polyanhydride nanoparticles (NPs) are a particularly attractive nano-carrier option in the context of CNS delivery due to their surface-eroding characteristics and superior internalization properties. In this work, a polyanhydride chemistry containing 1,6-bis(p-carboxyphenoxy)hexane and sebacic acid (i.e., 20:80 CPH:SA) was functionalized with (3-carboxypropyl)-triphenylphosphonium, a derivative of triphenylphosphonium which can target mitochondria and the blood brain barrier (BBB). The development of this bulk functionalization method is important for surface-eroding NPs to enable the persistence of the targeting ligand with the NPs throughout degradation for effective targeting of the hurdles downstream of the BBB. Surface-functionalized ligands may not be able to target these hurdles because they would be released from the NP too quickly after the onset of degradation in the body.
Studies in a rat mesencephalic neuronal cell line, N27, demonstrated significantly enhanced internalization of these bulk-functionalized NPs compared to non-functionalized 20:80 CPH:SA NPs as evaluated by flow cytometry and confocal microscopy. The ability of functionalized, drug-encapsulated NPs to improve the protective capability of the antioxidant Mito-apocynin against oxidative stress was also evaluated. Protection against oxidative stress by Mito-apocynin-encapsulated functionalized NPs was observed after challenging N27 cells with hydrogen peroxide, a known oxidative stress-inducing agent. These NPs were also dose-sparing compared to free drug. Taken altogether, these studies indicate the promise of this functionalization method for polyanhydride NPs and lay the foundation for improving therapeutic delivery to the brain.