Abstract

The long-term goal of this project is to develop a molecular, mechanistic approach to drug targeting. The central hypothesis of this research is: Prodrugs can be targeted to cells over expressing transporters and/or activating (hydrolytic) enzymes to achieve enhanced therapeutic efficacy. The approach utilizes the rapidly advancing knowledge in the areas of genomics, proteomics, and their respective databases, that will greatly facilitate the identification of membrane transporters and activating enzymes responsible for transport and activation of prodrugs.
The specific aims of this proposal are: 1: Synthesize a range of aliphatic, aromatic, acidic, basic imino, acidic, and basic, amino acid peptidomimetic prodrugs of floxuridine, gemcitabine and eladribine. 2: Evaluate the prodrugs in vitro for their solution and enzymatic hydrolysis, transport activity and cell growth inhibition activity. 3: Characterize the substrate specificity of BPHL with anticancer prodrugs and correlate with a homology model, produce the enzyme in amounts necessary for structural studies and determine the presence and identity of other prodrug activating enzymes from cancer cells. 4: Correlate the expression levels of transporters and enzymes involved in transport and activation of selected prodrugs in cancer cell lines and correlate with measured transport, prodrug activation and tumor growth inhibition activity. Evaluate two prodrug candidates in vivo for each parent drug for targeting potential and correlation with in vitro activity. This proposal will take advantage of the broad specificity of hPEPT1 (and other transporters) for nucleoside analogue prodrugs, and of our very exciting recent finding of an enzyme, valacyclovir hydrolase (BPHL), that activates the prodrugs valcyclovir and valganciclovir. We will develop and apply a molecular mechanistic approach to drug targeting, based on these findings and test this strategy in vivo with prodrugs of known anticancer agents. These studies will develop molecular mechanistic approaches for targeting anticancer prodrugs. The targeting approach and methods as well as structure-activity correlations developed in this project will be broadly applicable to the development of targeting strategies for other disease states and would be of immense value in optimizing drug discovery and development processes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM037188-20
Application #
7188058
Study Section
Pharmacology A Study Section (PHRA)
Program Officer
Okita, Richard T
Project Start
1986-09-01
Project End
2008-02-29
Budget Start
2007-03-01
Budget End
2008-02-29
Support Year
20
Fiscal Year
2007
Total Cost
$371,966
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Pharmacology
Type
Schools of Pharmacy
DUNS #
073133571
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Sun, Kefeng; Xu, Hao; Hilfinger, John L et al. (2018) Improved Protease-Targeting and Biopharmaceutical Properties of Novel Prodrugs of Ganciclovir. Mol Pharm 15:410-419
Incecayir, Tuba; Sun, Jing; Tsume, Yasuhiro et al. (2016) Carrier-Mediated Prodrug Uptake to Improve the Oral Bioavailability of Polar Drugs: An Application to an Oseltamivir Analogue. J Pharm Sci 105:925-934
Xu, Hao; Majmudar, Jaimeen D; Davda, Dahvid et al. (2015) Substrate-Competitive Activity-Based Profiling of Ester Prodrug Activating Enzymes. Mol Pharm 12:3399-407
Dahan, Arik; Wolk, Omri; Yang, Peihua et al. (2014) Dipeptidyl peptidase IV as a potential target for selective prodrug activation and chemotherapeutic action in cancers. Mol Pharm 11:4385-94
Walls, Zachary F; Gupta, Sheeba Varghese; Amidon, Gordon L et al. (2014) Synthesis and characterization of valyloxy methoxy luciferin for the detection of valacyclovirase and peptide transporter. Bioorg Med Chem Lett 24:4781-4783
Tsume, Yasuhiro; Incecayir, Tuba; Song, Xueqin et al. (2014) The development of orally administrable gemcitabine prodrugs with D-enantiomer amino acids: enhanced membrane permeability and enzymatic stability. Eur J Pharm Biopharm 86:514-23
Tsume, Yasuhiro; Mudie, Deanna M; Langguth, Peter et al. (2014) The Biopharmaceutics Classification System: subclasses for in vivo predictive dissolution (IPD) methodology and IVIVC. Eur J Pharm Sci 57:152-63
Xu, Hao; Sabit, Hairat; Amidon, Gordon L et al. (2013) An improved synthesis of a fluorophosphonate-polyethylene glycol-biotin probe and its use against competitive substrates. Beilstein J Org Chem 9:89-96
Incecayir, Tuba; Tsume, Yasuhiro; Amidon, Gordon L (2013) Comparison of the permeability of metoprolol and labetalol in rat, mouse, and Caco-2 cells: use as a reference standard for BCS classification. Mol Pharm 10:958-66
Gupta, Deepak; Varghese Gupta, Sheeba; Dahan, Arik et al. (2013) Increasing oral absorption of polar neuraminidase inhibitors: a prodrug transporter approach applied to oseltamivir analogue. Mol Pharm 10:512-22

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