Alcoholism and opiate addiction lead to major health-related problems and societal costs for people in the United States and the rest of the world as well. Therefore, research and development for improved pharmacologic treatments for drug and alcohol abuse are very important. Naltrexone, an opioid antagonist, is currently used in oral tablet form to help maintain opioid addicts in a drug-free state. Most recently, naltrexone has been indicated as an adjunct in the treatment of alcohol dependence, as well as reported to reduce alcohol craving in certain alcoholic populations. Transdermal delivery of naltrexone is desirable for opioid addicts and alcoholics in order to help reduce side effects associated with oral therapy and improve compliance. Naltrexone itself does not have the essential physicochemical properties that would allow a therapeutic dose of the drug to cross the human skin barrier. We plan to continue designing and synthesizing prodrugs, which are more skin permeable than naltrexone, in order to make a therapeutically successful drug delivery system. We hypothesize that prodrugs of naltrexone and prodrugs in combination with microneedle treatment will improve the transdermal delivery rate of naltrexone, and that these prodrugs will make excellent research tools for investigating quantitative structure-permeability relationships (QSPR) for transdermal flux and optimization of flux in combination with microneedle enhancement. These prodrugs/microneedles should improve naltrexone delivery rates across the skin because of optimized physicochemical properties for faster diffusion.
The specific aims of this project include: (1) to synthesize a series of naltrexone and naltrexol (active metabolite) prodrugs designed to elucidate fundamental QSPRs for transdermal flux optimization with and without microneedle use, (2) to characterize the physicochemical parameters of the drugs, including molecular weight, molecular volume, lipophilicity, hydrogen-bonding potentials, melting points, heats of fusion, and solubilities in select solvents, (3) to measure the drugs'penetration and concurrent bioconversion through human skin in vitro with and without microneedle use, and (4) to characterize the pharmacokinetics of the drugs in guinea pigs in vivo with and without microneedle use. Correlation of our in vitro data with the in vivo model will aid in the creation of a reliable QSPR database for transdermal prodrugs with and without microneedle use, as well as help to identify the most promising prodrug/microneedle system for eventual human use.

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA013425-06
Application #
7597157
Study Section
Human Development Research Subcommittee (NIDA)
Program Officer
Park, Moo Kwang
Project Start
2000-07-01
Project End
2011-03-31
Budget Start
2009-04-01
Budget End
2010-03-31
Support Year
6
Fiscal Year
2009
Total Cost
$310,666
Indirect Cost
Name
University of Kentucky
Department
Pharmacology
Type
Schools of Pharmacy
DUNS #
939017877
City
Lexington
State
KY
Country
United States
Zip Code
40506
Eldridge, Joshua A; Milewski, Mikolaj; Stinchcomb, Audra L et al. (2014) Synthesis and in vitro stability of amino acid prodrugs of 6-?-naltrexol for microneedle-enhanced transdermal delivery. Bioorg Med Chem Lett 24:5212-5
Ghosh, Priyanka; Lee, DoMin; Kim, Kyung Bo et al. (2014) Optimization of naltrexone diclofenac codrugs for sustained drug delivery across microneedle-treated skin. Pharm Res 31:148-59
Ghosh, Priyanka; Brogden, Nicole K; Stinchcomb, Audra L (2014) Fluvastatin as a micropore lifetime enhancer for sustained delivery across microneedle-treated skin. J Pharm Sci 103:652-60
Brogden, Nicole K; Banks, Stan L; Crofford, Leslie J et al. (2013) Diclofenac enables unprecedented week-long microneedle-enhanced delivery of a skin impermeable medication in humans. Pharm Res 30:1947-55
Ghosh, Priyanka; Brogden, Nicole K; Stinchcomb, Audra L (2013) Effect of formulation pH on transport of naltrexone species and pore closure in microneedle-enhanced transdermal drug delivery. Mol Pharm 10:2331-9
Ghosh, Priyanka; Pinninti, Raghotham R; Hammell, Dana C et al. (2013) Development of a codrug approach for sustained drug delivery across microneedle-treated skin. J Pharm Sci 102:1458-67
Milewski, Mikolaj; Paudel, Kalpana S; Brogden, Nicole K et al. (2013) Microneedle-assisted percutaneous delivery of naltrexone hydrochloride in yucatan minipig: in vitro-in vivo correlation. Mol Pharm 10:3745-57
Brogden, Nicole K; Ghosh, Priyanka; Hardi, Lucia et al. (2013) Development of in vivo impedance spectroscopy techniques for measurement of micropore formation following microneedle insertion. J Pharm Sci 102:1948-1956
Brogden, Nicole K; Milewski, Mikolaj; Ghosh, Priyanka et al. (2012) Diclofenac delays micropore closure following microneedle treatment in human subjects. J Control Release 163:220-9
Milewski, Mikolaj; Pinninti, Raghotham R; Stinchcomb, Audra L (2012) Naltrexone salt selection for enhanced transdermal permeation through microneedle-treated skin. J Pharm Sci 101:2777-86

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