Literature DB >> 3801051

Enhanced melphalan cytotoxicity in human ovarian cancer in vitro and in tumor-bearing nude mice by buthionine sulfoximine depletion of glutathione.

R F Ozols, K G Louie, J Plowman, B C Behrens, R L Fine, D Dykes, T C Hamilton.   

Abstract

The development of acquired resistance to alkylating agents frequently limits the effectiveness of chemotherapy in the treatment of ovarian cancer. While the resistance to alkylating agents is multifactorial, the association of drug resistance with elevations in glutathione (GSH) is of potential clinical relevance since there exist pharmacologic means to lower intracellular GSH levels. We have used in vitro and in vivo models of human ovarian cancer to demonstrate that selective inhibition of GSH synthesis with L-buthionine-S,R-sulfoximine (L-BSO) leads to a lowering of GSH levels and an increase in cytotoxicity of the alkylating agent melphalan. In the human ovarian cancer cell line NIH:OVCAR-3, derived from a patient clinically refractory to alkylating agents, L-BSO resulted in a 3.6-fold enhancement of melphalan cytotoxicity. This cell line was also adapted for intraperitoneal growth in athymic nude mice. In this in vivo model, in which the mice die of massive ascites and intraabdominal carcinomatosis, L-BSO given orally in drinking water for 5 days decreased GSH levels in the tumor cells by 96% compared to a 79 and 86% reduction in GSH levels in the bone marrow and gastrointestinal mucosa respectively. Lowering of GSH levels with BSO was not accompanied by an increase in lethality for melphalan in non-tumored nude mice. However, in tumor-bearing nude mice, a single melphalan (5 mg/kg) treatment following GSH depletion with L-BSO was markedly superior to treatment with melphalan alone, producing a 72% increase in median survival time. Furthermore, L-BSO treatment of human bone marrow cells prior to melphalan exposure had little effect on melphalan toxicity as assessed in a CFUc-GM assay. These results suggest that treatment with the GSH synthesis inhibitor BSO may preferentially enhance the cytotoxic effects of alkylating agents against human ovarian cancer and overcome acquired resistance.

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Year:  1987        PMID: 3801051     DOI: 10.1016/0006-2952(87)90392-3

Source DB:  PubMed          Journal:  Biochem Pharmacol        ISSN: 0006-2952            Impact factor:   5.858


  28 in total

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4.  Effect of selenium compounds and thiols on human mammary tumor cells.

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5.  Intra-arterial chemotherapy with osmotic blood-brain barrier disruption for aggressive oligodendroglial tumors: results of a phase I study.

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Review 6.  Systemic chemotherapy for malignant melanoma.

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7.  Melphalan-induced toxicity in nude mice following pretreatment with buthionine sulfoximine.

Authors:  S X Skapek; A F VanDellen; D P McMahon; D G Postels; O W Griffith; D D Bigner; H S Friedman
Journal:  Cancer Chemother Pharmacol       Date:  1991       Impact factor: 3.333

8.  Buthionine sulfoximine induced growth inhibition in human lung carcinoma cells does not correlate with glutathione depletion.

Authors:  Y J Kang; D Emery; M D Enger
Journal:  Cell Biol Toxicol       Date:  1991-07       Impact factor: 6.691

9.  Selenite-induced inhibition of colony formation by buthionine sulfoximine-sensitive and resistant cell lines.

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10.  Development of a model of melphalan-induced gastrointestinal toxicity in mice.

Authors:  S Castellino; G B Elion; O W Griffith; M Dewhirst; J Kurtzberg; R C Cattley; P Scott; D D Bigner; H S Friedman
Journal:  Cancer Chemother Pharmacol       Date:  1993       Impact factor: 3.333

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