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pubmed-article:2706620pubmed:abstractTextFour of seven human melanoma cell lines were sensitive to killing by L-dopa (D37 1.0-4.7 microM) compared with fibroblasts, Hela, and three ovarian tumor cell lines (D37 12-59 microM). All seven melanoma lines, however, were sensitive to DL-buthionine(S,R)sulfoximine (BSO) (D37 0.73-8.5 microM) compared with the nonmelanoma cells (D37 25-68 microM). The melanoma line most sensitive to BSO (MM418) was highly melanized, proliferated slowly and was resistant to other agents [dopa, 5-(3-methyl-1-triazeno)5-imidazole-4-carboxamide, melphalan, methotrexate, hydroxyurea, etoposide, Adriamycin]. In most cell lines, L-dopa and BSO blocked cell proliferation in all phases of the cell cycle. Cellular sensitivity to dopa or BSO did not correlate with levels of total soluble SH, glutathione (GSH), GSH reductase, GSH peroxidase or GSH transferase, or with the extent of GSH depletion induced by the drug. No GSH transferase activity could be detected in the dopa-resistant HeLa line, indicating that detoxification of quinones is not an important mechanism of resistance. Within the group of melanoma cell lines, sensitivity to dopa correlated with decreased level of gamma-glutamyl transpeptidase (r = 0.81). However, the gamma-glutamyl transpeptidase inhibitor azaserine was less effective than BSO in enhancing the toxicity of dopa. It can be inferred that (a) there is no simple relationship between GSH metabolism and sensitivity to dopa or BSO in human melanoma cells, and (b) BSO may be an effective agent for melanoma.lld:pubmed
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pubmed-article:2706620pubmed:dateRevised2006-11-15lld:pubmed
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pubmed-article:2706620pubmed:year1989lld:pubmed
pubmed-article:2706620pubmed:articleTitleSensitivity of human melanoma cells to L-dopa and DL-buthionine (S,R)-sulfoximine.lld:pubmed
pubmed-article:2706620pubmed:affiliationQueensland Institute of Medical Research, Herston, Australia.lld:pubmed
pubmed-article:2706620pubmed:publicationTypeJournal Articlelld:pubmed
pubmed-article:2706620pubmed:publicationTypeResearch Support, Non-U.S. Gov'tlld:pubmed