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Dual-functionalisation of gelatine nanoparticles with an anticancer platinum(II)-bisphosphonate complex and mineral-binding alendronate

Academic Article
Publication Date:
2016
abstract:
In order to improve the efficacy of therapeutic systems to treat bone tumours, novel drug delivery vehicles should be developed that have strong and specific affinity to mineralised tissue and at the same time are able to release anticancer molecules locally in a controlled and sustained manner. Recently, we developed mineral-binding gelatine nanoparticles with enhanced affinity to calcium phosphate by conjugating alendronate (ALN) molecules onto their surface. Herein, we have enhanced the functionality of these nanoparticles by rendering them potentially therapeutically active via covalent linking of an anticancer platinum-bisphosphonate (Pt-BP) complex. Different functionalisation schemes and molar ratios between reactants were screened and the effective functionalisation of gelatine nanoparticles with Pt-BP (or with both Pt-BP and ALN) was assessed. Our results revealed that the degree of functionalisation could be tailored by varying the molar ratio of Pt-BP and ALN relative to glutaraldehyde used as crosslinker. A sustained and tunable release of platinum as a function of the initial Pt-BP/ALN/ glutaraldehyde molar ratio was achieved for both Pt-BP-and dual-functionalised gelatine nanoparticles. Moreover, dual-functionalised gelatine nanoparticles also displayed a high affinity to hydroxyapatitecoated surfaces thanks to the presence of ALN. Summarising, it was demonstrated that mineral-binding gelatine nanoparticles can be loaded with tailored amounts of anticancer molecules, which may benefit the development of bone-seeking carriers for targeted delivery of drugs to treat bone tumours.
Iris type:
01.01 Articolo in rivista
Keywords:
platinum-bisphosphonate; alendronate; mineral-binding; conjugation; gelatin nanoparticles; targeted delivery; bone tumor
List of contributors:
Iafisco, Michele
Authors of the University:
IAFISCO MICHELE
Handle:
https://iris.cnr.it/handle/20.500.14243/356521
Published in:
RSC ADVANCES
Journal
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