Abstract

Methyl and ethyl thioether groups were introduced at all primary positions of α-, β-, and γ-cyclodextrin by nucleophilic displacement reactions starting from the corresponding per-(6-deoxy-6-bromo)cyclodextrins. Further modification of all 2-OH positions by etherification with iodo terminated triethylene glycol monomethyl ether (and tetraethylene glycol monomethyl ether, respectively) furnished water-soluble hosts. Especially the β-cyclodextrin derivatives exhibit very high binding potentials towards the anaesthetic drugs sevoflurane and halothane. Since the resulting inclusion compounds are highly soluble in water at temperatures ≤37 °C they are good candidates for new aqueous dosage forms which would avoid inhalation anaesthesia.

Highlights

  • Cyclodextrins (CDs) are cyclic oligomers of α-1,4-linked glucose units

  • Methyl and ethyl thioether groups were introduced at all primary positions of α, β, and γ-cyclodextrin by nucleophilic displacement reactions starting from the corresponding per-(6-deoxy-6-bromo)cyclodextrins

  • CDs are well known to increase the bioavailability of active pharmaceutical ingredients (APIs) [2,3], and they are readily available in pharmaceutical purity and industrial quantities

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Summary

Introduction

Cyclodextrins (CDs) are cyclic oligomers of α-1,4-linked glucose units. CDs are well known to increase the bioavailability of active pharmaceutical ingredients (APIs) [2,3], and they are readily available in pharmaceutical purity and industrial quantities. They are water soluble and regarded as non-toxic in case of α- and γ-CD [4,5], while β-CD shows some toxic effects such as haemolysis at high concentrations [6]. CDs are generally employed to increase the bioavailability of those APIs scarcely soluble in water [7]. There are several formulations of APIs containing CDs on the market, such as prostaglandine/α-CD [8], and piroxicam/β-CD [9]

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