Functionalization of Cyclodextrin Derivatives to Create Supramolecular Pharmaceutical Materials

Abstract

Molecular recognition is useful in creating functional supramolecular materials. Non-covalent bond formations, such as host-guest interactions, hydrogen bonding, and electrostatic interaction, are effective tools for introducing various functions and properties into materials. This review focuses on such macroscopic functions as selective molecular adhesion, self-healing, toughness, and the actuation of supramolecular polymeric materials-materials which have potential in pharmaceutical development. These functions have been achieved using reversible bonding between cyclodextrins (CDs; cyclic host molecules) and guest molecules. For example, macroscopic adhesions between host-modified hydrogels and guest-modified hydrogels have been investigated. CD-modified hydrogels were found to show selective adhesion to a guest hydrogel with an appropriate molecular size for the CD cavity, indicating that the host-guest complex formation between the gels led to the adhesive behavior. Surprisingly, polymeric materials having host-guest cross-linking points show both high toughness and flexibility, unlike conventional covalently cross-linked materials. These materials also exhibited self-healing properties, capable of repairing damage to the materials. Furthermore, the supramolecular materials demonstrated macroscopic rapid expansion and contraction driven by external stimuli under wet or semi-dry conditions, in which the supramolecular gels vary the cross-linking density between the polymers accordingly. Different topological gels are able to vary the length of the polymer chain between cross-linking points to show large deformation. Both types of actuators were found to exhibit externally stimulated flexing behaviors. This review summarizes recent advancements in the development of these supramolecular materials, which appear to be promising new components in pharmaceutical science.