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pH-Dependent silica nanoparticle dissolution and cargo release

Giovaninni, Giorgia, Moore, Colin J., Hall, Andrew J., Byrne, Hugh J., Gubala, Vladimir (2018) pH-Dependent silica nanoparticle dissolution and cargo release. Colloids and Surfaces B: Biointerfaces, 169 . pp. 242-248. ISSN 0927-7765. (doi:10.1016/j.colsurfb.2018.04.064) (KAR id:67094)

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The dissolution of microporous silica nanoparticles (NP) in aqueous environments of different biologically relevant pH was studied in order to assess their potential as drug delivery vehicles. Silica NPs, loaded with fluorescein, were prepared using different organosilane precursors (tetraethoxysilane, ethyl triethoxysilane or a 1:1 molar ratio of both) and NP dissolution was evaluated in aqueous conditions at pH 4, pH 6 and pH 7.4. These conditions correspond to the acidity of the intracellular environment (late endosome, early endosome, cytosol respectively) and gastrointestinal tract (‘fed’ stomach, duodenum and jejunum respectively). All NPs degraded at pH 6 and pH 7.4, while no dissolution was observed at pH 4. NP dissolution could be clearly visualised as mesoporous hollows and surface defects using electron microscopy, and was supported by UV–vis, fluorimetry and DLS data. The dissolution profiles of the NPs are particularly suited to the requirements of oral drug delivery, whereby NPs must resist degradation in the harsh acidic conditions of the stomach (pH 4), but dissolve and release their cargo in the small intestine (pH 6–7.4). Particle cores made solely of ethyl triethoxysilane exhibited a ‘burst release’ of encapsulated fluorescein at pH 6 and pH 7.4, whereas NPs synthesised with tetraethoxysilane released fluorescein in a more sustained fashion. Thus, by varying the organosilane precursor used in NP formation, it is possible to modify particle dissolution rates and tune the release profile of encapsulated fluorescein. The flexible synthesis afforded by silica NPs to achieve pH-responsive dissolution therefore makes this class of nanomaterial an adaptable platform that may be well suited to oral delivery applications.

Item Type: Article
DOI/Identification number: 10.1016/j.colsurfb.2018.04.064
Uncontrolled keywords: Microporous, Nanoparticle, Silica, Dissolution, Intracellular, Dye release, Drug delivery, Oral delivery
Divisions: Divisions > Division of Natural Sciences > Medway School of Pharmacy
Depositing User: Vladimir Gubala
Date Deposited: 21 May 2018 09:40 UTC
Last Modified: 16 Feb 2021 13:54 UTC
Resource URI: (The current URI for this page, for reference purposes)
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