Abstract

Camptothecin and related analogues display unprecedented antitumor activities against a variety of human cancers. To date the full therapeutic utilities of these agents have been limited by the aqueous instability of their lactone ring moiety, with the intactness of this pharmacophore an essential requirement for antitumor activity. For each drug ring opening is rapid under physiological condiitons (i.el, pH 7.0 or above), resulting in a complete loss of biological activity. In recently completed investigations [Burke et al., Journal of the American Chemical Society 114:8318-8314, (1992); Burke et al., Biochemistry 32:5352-5364, (1993)], we have demonstrated that liposome-bound camptothecin drugs are stable. Liposome stability data presented herein suggest that liposomes may potentially serve as carriers of camptothecin drugs which conserve both lactone ring and enhance antitumor activities. The present proposal is a four-year study aimed at evaluating the cellular pharmacology, blood stability, antitumor activity, toxicity, pharmacokinetics, organ distribution and tumor uptake of several prototype liposomal preparations of newly-synthesized lipophilic camptothecins. Despite favorable findings over the past ten years indicating that the more lipophilic camptothecin analogues are the most potent compounds against experimental cancers including multidrug-resistant (MDR) phenotypes, their further development has been sidetracked due to formulation problems. However, our recent experiments clearly show that liposomal formulations result in both enhanced drug stability and marked improvements in antitumor activity. Such an approach allows the liposomes to both solubilize and stabilize the drugs. The concept of liposomal drug delivery is an intriguing one in that it opens the door to the further development and evaluation of lipophilic camptothecins such as 10,11- methylenedioxycamptothecin more potent and MDR-active than water-soluble analogues such as 9-aminocamptothecin, topotecan, and CPT-11. Liposome formulations stabilize and enhance the in vitro antitumor activities of camptothecins; thus they may be of potential utility for introducing this promising class of anticancer agents to cancer victims. We propose here to explore the feasibility of liposomes as drug delivery vehicles for lipophilic analogues.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
1R01CA063653-01
Application #
2105633
Study Section
Experimental Therapeutics Subcommittee 1 (ET)
Project Start
1994-05-01
Project End
1998-02-28
Budget Start
1994-05-01
Budget End
1995-02-28
Support Year
1
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
Ohio State University
Department
Type
Schools of Pharmacy
DUNS #
098987217
City
Columbus
State
OH
Country
United States
Zip Code
43210

  Publications

Song, Lin; Bevins, Robert; Anderson, Bradley D (2006) Kinetics and mechanisms of activation of alpha-amino acid ester prodrugs of camptothecins. J Med Chem 49:4344-55
Lopez-Barcons, Lluis A; Zhang, Junhong; Siriwitayawan, Gunching et al. (2004) The novel highly lipophilic topoisomerase I inhibitor DB67 is effective in the treatment of liver metastases of murine CT-26 colon carcinoma. Neoplasia 6:457-67
Liu, Xinli; Zhang, Junhong; Song, Lin et al. (2004) Degradation of camptothecin-20(S)-glycinate ester prodrug under physiological conditions. J Pharm Biomed Anal 35:1113-25
Du, Wu; Curran, Dennis P; Bevins, Robert L et al. (2002) Synthesis and evaluation of a novel E-ring modified alpha-hydroxy keto ether analogue of camptothecin. Bioorg Med Chem 10:103-10
Liu, Xinli; Lynn, Bert C; Zhang, Junhong et al. (2002) A versatile prodrug approach for liposomal core-loading of water-insoluble camptothecin anticancer drugs. J Am Chem Soc 124:7650-1
Bom, D; Curran, D P; Zhang, J et al. (2001) The highly lipophilic DNA topoisomerase I inhibitor DB-67 displays elevated lactone levels in human blood and potent anticancer activity. J Control Release 74:325-33
Bom, D; Curran, D P; Kruszewski, S et al. (2000) The novel silatecan 7-tert-butyldimethylsilyl-10-hydroxycamptothecin displays high lipophilicity, improved human blood stability, and potent anticancer activity. J Med Chem 43:3970-80
Bom, D; Curran, D P; Chavan, A J et al. (1999) Novel A,B,E-ring-modified camptothecins displaying high lipophilicity and markedly improved human blood stabilities. J Med Chem 42:3018-22
Pollack, I F; Erff, M; Bom, D et al. (1999) Potent topoisomerase I inhibition by novel silatecans eliminates glioma proliferation in vitro and in vivo. Cancer Res 59:4898-905
Shenderova, A; Burke, T G; Schwendeman, S P (1999) The acidic microclimate in poly(lactide-co-glycolide) microspheres stabilizes camptothecins. Pharm Res 16:241-8

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