The chemical reactivity of as-anodized porous silicon is shown to have an adverse effect on a model drug (Lansoprazole) loaded into the pores. The silicon hydride surfaces can cause unwanted reactions with actives during storage or use. Techniques such as thermal oxidation or surface derivitization can lower the reactivity somewhat, by replacing the reactive silicon-hydride species with a more benign oxide or functional group. However, by using a trio of analytical techniques (fluorometric dye assay, HPLC assay, and chemography) we show that residual hydride is still likely to be present and only after combining thermal oxidation with surface derivitization can the residual reactivity be reduced to those values typically observed with sol-gel (porous) silica. Potential sources of residual reactivity are discussed, with reference to data obtained by trace metal analysis, residual solvents, and pH measurements.

Quantification and Reduction of the Residual Chemical Reactivity of Passivated Biodegradable Porous Silicon for Drug Delivery Applications

De Stefano L;Rea I
2018

Abstract

The chemical reactivity of as-anodized porous silicon is shown to have an adverse effect on a model drug (Lansoprazole) loaded into the pores. The silicon hydride surfaces can cause unwanted reactions with actives during storage or use. Techniques such as thermal oxidation or surface derivitization can lower the reactivity somewhat, by replacing the reactive silicon-hydride species with a more benign oxide or functional group. However, by using a trio of analytical techniques (fluorometric dye assay, HPLC assay, and chemography) we show that residual hydride is still likely to be present and only after combining thermal oxidation with surface derivitization can the residual reactivity be reduced to those values typically observed with sol-gel (porous) silica. Potential sources of residual reactivity are discussed, with reference to data obtained by trace metal analysis, residual solvents, and pH measurements.
2018
Porous silicon
Reactivity
Derivatization
Drug delivery
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/20.500.14243/425344
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