An inclusion complex of hydroxymethylferrocene (FeMeOH) with β-cyclodextrin (β-CD) was prepared in the solid state by different techniques such as physical mixture, coprecipitation, kneading and freeze-drying. The formation of the inclusion complex was confirmed by X-ray Powder Diffractometry and Fourier Transform- Infrared spectroscopy. In aqueous solution, the 1:1 stoichiometry was established by a Job plot. The inclusion complex formation was also investigated by NMR and the stability constant (K b) of the complex was determined to be 478 M -1, which is in agreement with that obtained with UV-Vis tritation (K b = 541.3 M -1). The phase solubility study showed a diagram classified as BS type and that the solubility of FeMeOH was slightly increased in the presence of β-CD. Furthermore, utilizing phase solubility diagram data, the K b was estimated to be equal to 528.0 M -1. The cytotoxic activity of FeMeOH and its complexation product with β-CD was determined using the MTT-assay on MDA-MB-231 cell line, showing that the inclusion complex has a higher capability of inhibiting cell growth compared to that of pure FeMeOH. © 2012 by the Authors.

Physicochemical Characterization and Cytotoxic Activity Evaluation of Hydroxymethylferrocene:beta-Cyclodextrin Inclusion Complex

IACOVINO, Rosa;ISIDORI, Marina;LAVORGNA, Margherita;MALGIERI, Gaetano;ISERNIA, Carla
2012

Abstract

An inclusion complex of hydroxymethylferrocene (FeMeOH) with β-cyclodextrin (β-CD) was prepared in the solid state by different techniques such as physical mixture, coprecipitation, kneading and freeze-drying. The formation of the inclusion complex was confirmed by X-ray Powder Diffractometry and Fourier Transform- Infrared spectroscopy. In aqueous solution, the 1:1 stoichiometry was established by a Job plot. The inclusion complex formation was also investigated by NMR and the stability constant (K b) of the complex was determined to be 478 M -1, which is in agreement with that obtained with UV-Vis tritation (K b = 541.3 M -1). The phase solubility study showed a diagram classified as BS type and that the solubility of FeMeOH was slightly increased in the presence of β-CD. Furthermore, utilizing phase solubility diagram data, the K b was estimated to be equal to 528.0 M -1. The cytotoxic activity of FeMeOH and its complexation product with β-CD was determined using the MTT-assay on MDA-MB-231 cell line, showing that the inclusion complex has a higher capability of inhibiting cell growth compared to that of pure FeMeOH. © 2012 by the Authors.
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11591/322305
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