Topical Cream-Based Dosage Forms of the Macrocyclic Drug Delivery Vehicle Cucurbit[6]uril
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Open Access
Type
ArticleAbstract
The macrocycle family of molecules called cucurbit[n]urils are potential drug delivery vehicles as they are able to form hostguest complexes with many different classes of drugs. This study aimed to examine the utility of cucurbit[6]uril (CB[6]) in topical cream-based formulations ...
See moreThe macrocycle family of molecules called cucurbit[n]urils are potential drug delivery vehicles as they are able to form hostguest complexes with many different classes of drugs. This study aimed to examine the utility of cucurbit[6]uril (CB[6]) in topical cream-based formulations for either localised treatment or for transdermal delivery. Cucurbit[6]uril was formulated into both buffered cream aqueous- and oily cream-based dosage forms. The solid state interaction of CB[6] with other excipients was studied by differential scanning calorimetry and the macrocycle’s transdermal permeability was determined using rat skin. Significant solid state interactions were observed between CB[6] and the other dosage form excipients. At concentrations up to 32% w/w the buffered aqueous cream maintained its normal consistency and could be effectively applied to skin, but the oily cream was too stiff and is not suitable as a dosage form. Cucurbit[6]uril does not permeate through skin; as such, the results imply that cucurbituril-based topical creams may potentially only have applications for localised skin treatment and not for transdermal drug delivery.
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See moreThe macrocycle family of molecules called cucurbit[n]urils are potential drug delivery vehicles as they are able to form hostguest complexes with many different classes of drugs. This study aimed to examine the utility of cucurbit[6]uril (CB[6]) in topical cream-based formulations for either localised treatment or for transdermal delivery. Cucurbit[6]uril was formulated into both buffered cream aqueous- and oily cream-based dosage forms. The solid state interaction of CB[6] with other excipients was studied by differential scanning calorimetry and the macrocycle’s transdermal permeability was determined using rat skin. Significant solid state interactions were observed between CB[6] and the other dosage form excipients. At concentrations up to 32% w/w the buffered aqueous cream maintained its normal consistency and could be effectively applied to skin, but the oily cream was too stiff and is not suitable as a dosage form. Cucurbit[6]uril does not permeate through skin; as such, the results imply that cucurbituril-based topical creams may potentially only have applications for localised skin treatment and not for transdermal drug delivery.
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Date
2014-01-15Publisher
Public Library of ScienceLicence
OtherFaculty/School
Faculty of Medicine and Health, Sydney Pharmacy SchoolCitation
Seif M, Impelido ML, Apps MG, Wheate NJ (2014) Topical Cream-Based Dosage Forms of the Macrocyclic Drug Delivery Vehicle Cucurbit[6]uril. PLoS ONE 9(1): e85361Share