Literature DB >> 20858066

Transdermal permeation of novel n-acetyl-glucosamine/NSAIDs mutual prodrugs.

Bridg'ette Israel1, Solomon T Garner, Mohan Thakare, Deborah Elder, Trinia Abney, Parastoo Azadi, J Warren Beach, James C Price, Hisham Ahmed, Anthony C Capomacchia.   

Abstract

The current investigation reports skin permeation of three novel mutual prodrugs (MP) which couple n-acetyl-glucosamine with an NSAID, either ketoprofen or ibuprofen. They were evaluated for transdermal permeation using shed snakeskin, and to our knowledge represent the first MPs synthesized for this purpose, although they also could be used for subcutaneous delivery. MPs are defined as two active drug compounds usually connected by an ester linkage. Glucosamine administration has been linked to damaged cartilage repair, and pain relief in joints afflicted with osteoarthritis. NSAIDs are commonly used orally in transdermal creams or gels for joint pain relief. Two novel compounds we report (MP1 and MP2) covalently link ibuprofen and ketoprofen directly to the amide nitrogen of n-acetyl-glucosamine (NAG); the other compound (MP3) covalently links ibuprofen to the amide nitrogen, using a short chain acetyl linker. Permeability studies show that the ketoprofen mutual prodrug (MP2) permeates shed snakeskin more than three times greater than either ibuprofen derivative, while ethanol markedly increases the permeation for all three. The ketoprofen mutual prodrug appears the most likely candidate for transdermal administration; all three mutual prodrugs may be candidates for subcutaneous injection.

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Year:  2010        PMID: 20858066     DOI: 10.3109/10837450.2010.513987

Source DB:  PubMed          Journal:  Pharm Dev Technol        ISSN: 1083-7450            Impact factor:   3.133


  1 in total

1.  Enhancing Skin Permeation of Biphenylacetic Acid (BPA) Using Salt Formation with Organic and Alkali Metal Bases.

Authors:  Vijay Pawar; Prashant Naik; Rajani Giridhar; Mange Ram Yadav
Journal:  Sci Pharm       Date:  2014-09-26
  1 in total

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