Publication | Open Access
Incorporation and Controlled Release of Silyl Ether Prodrugs from PRINT Nanoparticles
125
Citations
23
References
2012
Year
NanoparticlesNanotherapeuticsEngineeringPrint NanoparticlesChemistryProtein NanoparticlesNanomedicineChemical EngineeringMedicinal ChemistryPrinted ElectronicsDrug Delivery SystemSilyl Ether ProdrugsBiopolymersPharmacologyNm ParticlesNanomaterialsAbs ProdrugsPolymer-drug ConjugatePharmaceutical NanotechnologyDrug Delivery SystemsNano-drug DeliveryMedicineNovel NanoparticlesDrug DiscoveryDrug Analysis
Asymmetric bifunctional silyl ether (ABS) prodrugs of chemotherapeutics were synthesized and incorporated within 200 nm × 200 nm particles. ABS prodrugs of gemcitabine were selected as model compounds because of the difficulty to encapsulate a water-soluble drug within a hydrogel. The resulting drug delivery systems were degraded under acidic conditions and were found to release only the parent or active drug. Furthermore, changing the steric bulk of the alkyl substituents on the silicon atom could regulate the rate of drug release and, therefore, the intracellular toxicity of the gemcitabine-loaded particles. This yielded a family of novel nanoparticles that could be tuned to release drug over the course of hours, days, or months.
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