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Complexation in a β-cyclodextrin-salicylic acid system

Journal

COLLOID JOURNAL
Volume 69, Issue 5, Pages 546-551

Publisher

PLEIADES PUBLISHING INC
DOI: 10.1134/S1061933X0705002X

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Inclusion host-guest complexes are synthesized from beta-cyclodextrin and salicylic acid, which is a nonsteroid anti-inflammatory drug with a wide range of action. By IR and UV spectroscopy, and X-ray diffraction, and thermogravimetry, it is established that axial 1:1 complexes of the tail forward type are formed due to the dispersion interactions between internal hydrophobic cavities of beta-cyclodextrin molecules and salicylic acid aromatic rings. Salicylic acid is stabilized due to the fact that its carboxyl group is located in the plane of the upper edge of beta-cyclodextrin molecule and weak hydrogen bond is formed between phenyl hydroxyl and glycoside oxygen. The encapsulation of salicylic acid changes its crystal structure and thermal stability.

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