Abstract

During the last three years we have successfully synthesized various hydrotropic polymers, hydrogels, dendrimers, and polymeric micelles that achieve solubility enhancement by several orders of magnitude for paclitaxel, a notoriously poorly soluble anticancer drug. The preliminary in vivo data using hydrotropic polymeric micelles have indicated that the therapeutically effective blood concentration of paclitaxel can be achieved if all of the loaded paclitaxel can be released during the GI transit time. The goal of this project is to synthesize hydrotropic polymer micelles that produce highly stable aqueous formulations but at the same time release paclitaxel fast upon contact with gastric and intestinal fluids. The hypothesis to be tested in this project is that the water-solubility of paclitaxel by 2-4 orders of magnitude overcomes the adverse effect of P-glycoprotein (Pgp) to result in clinically significant bioavailability.
The specific aims are: (1) to synthesize hydrotropic polymer micelles with various affinities to paclitaxel for controlling the paclitaxel release kinetics and mucoadhesive or inverse thermo-sensitive micelles for enhancing the GI transit time; (2) to control the in vitro paclitaxel release kinetics from the oral formulations; (3) to evaluate the cytotoxic efficacy of the formulations using human tumor cell lines; and (4) to examine the in vivo bioavailability using an in vivo chronically catheterized rat model. Since the increased bioavailability is based on the faster release of paclitaxel in the GI tract, the potential GI toxicity of the paclitaxel formulations will be examined by testing gastrointestinal permeability and by histological examination of the intestinal tissues. The fast release of paclitaxel will be achieved by introducing pH- sensitive moiety into the hydrotropic block so that the affinity to paclitaxel can be lowered by simple pH changes. This project is expected to produce novel hydrotropic polymeric micelle systems that have high drug loading efficiency, high stability, and yet fast release of the loaded paclitaxel in the GI tract. This will provide a new avenue of paclitaxel delivery by oral administration. The oral paclitaxel formulations are expected to have great therapeutic potential not only for cancer treatment as well as neurodegenerative diseases that can be potentially treated by paclitaxel. ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM065284-05
Application #
7162121
Study Section
Gene and Drug Delivery Systems Study Section (GDD)
Program Officer
Okita, Richard T
Project Start
2002-04-01
Project End
2008-12-31
Budget Start
2007-01-01
Budget End
2007-12-31
Support Year
5
Fiscal Year
2007
Total Cost
$276,232
Indirect Cost

  Institution

Name
Purdue University
Department
Type
Schools of Pharmacy
DUNS #
072051394
City
West Lafayette
State
IN
Country
United States
Zip Code
47907

  Publications

Lu, Ying; Park, Kinam (2013) Polymeric micelles and alternative nanonized delivery vehicles for poorly soluble drugs. Int J Pharm 453:198-214
Lee, Seung-Young; Kim, Sungwon; Tyler, Jacqueline Y et al. (2013) Blood-stable, tumor-adaptable disulfide bonded mPEG-(Cys)4-PDLLA micelles for chemotherapy. Biomaterials 34:552-61
Park, Kinam (2013) Facing the truth about nanotechnology in drug delivery. ACS Nano 7:7442-7
Kim, Ji Young; Kim, Sungwon; Pinal, Rodolfo et al. (2011) Hydrotropic polymer micelles as versatile vehicles for delivery of poorly water-soluble drugs. J Control Release 152:13-20
Lu, Ying; Kim, Sungwon; Park, Kinam (2011) In vitro-in vivo correlation: perspectives on model development. Int J Pharm 418:142-8
Kim, Ji Young; Kim, Sungwon; Papp, Michelle et al. (2010) Hydrotropic solubilization of poorly water-soluble drugs. J Pharm Sci 99:3953-65
Kim, Sungwon; Kim, Jong-Ho; Jeon, Oju et al. (2009) Engineered polymers for advanced drug delivery. Eur J Pharm Biopharm 71:420-30
Kim, Sungwon; Kim, Ji Young; Huh, Kang Moo et al. (2008) Hydrotropic polymer micelles containing acrylic acid moieties for oral delivery of paclitaxel. J Control Release 132:222-9
Chen, Hongtao; Kim, Sungwon; He, Wei et al. (2008) Fast release of lipophilic agents from circulating PEG-PDLLA micelles revealed by in vivo forster resonance energy transfer imaging. Langmuir 24:5213-7
Huh, Kang Moo; Min, Hyun Su; Lee, Sang Cheon et al. (2008) A new hydrotropic block copolymer micelle system for aqueous solubilization of paclitaxel. J Control Release 126:122-9

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