Darinaparsin induces a unique cellular response and is active in an arsenic trioxide-resistant myeloma cell line

Here, we report on the organic arsenical darinaparsin (ZIO-101, S -dimethylarsino-glutathione) and its anti-myeloma activity compared with inorganic arsenic trioxide. Darinaparsin induced apoptosis in multiple myeloma cell lines in a dose-dependent manner, and the addition of N -acetylcysteine, whic...

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Bibliographic Details
Published in:Molecular cancer therapeutics 2009-05, Vol.8 (5), p.1197-1206
Main Authors: Matulis, Shannon M, Morales, Alejo A, Yehiayan, Lucy, Croutch, Claire, Gutman, Delia, Cai, Yong, Lee, Kelvin P, Boise, Lawrence H
Format: Article
Language:English
Subjects:
Antineoplastic Agents - pharmacology
Apoptosis - drug effects
Arsenic Trioxide
Arsenicals - metabolism
Arsenicals - pharmacology
Buthionine Sulfoximine - metabolism
Buthionine Sulfoximine - pharmacology
Cell Line, Tumor
Cell Survival - drug effects
Cysteine - metabolism
Cysteine - pharmacology
Darinaparsin
Drug Resistance, Neoplasm - drug effects
Gene Expression Profiling
Gene Expression Regulation, Neoplastic - drug effects
Glutathione
Glutathione - analogs & derivatives
Glutathione - metabolism
Glutathione - pharmacology
Humans
Multiple Myeloma - metabolism
Myeloma
Oxides - metabolism
Oxides - pharmacology
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Summary:Here, we report on the organic arsenical darinaparsin (ZIO-101, S -dimethylarsino-glutathione) and its anti-myeloma activity compared with inorganic arsenic trioxide. Darinaparsin induced apoptosis in multiple myeloma cell lines in a dose-dependent manner, and the addition of N -acetylcysteine, which increases intracellular glutathione (GSH), blocked cytotoxicity of both darinaparsin and arsenic trioxide. In contrast to arsenic trioxide, intracellular GSH does not appear to be important for darinaparsin metabolism, as an inhibitor of GSH synthesis, buthionine sulfoximine, had little effect on drug activity. This discrepancy was resolved when we determined the effects of thiols on drug uptake. The addition of exogenous GSH, l -cysteine, or d -cysteine prevented darinaparsin cellular uptake and cell death but had no effect on the uptake or activity of arsenic trioxide, suggesting a difference in the transport mechanism of these two drugs. In addition, gene expression profiling revealed differences in the signaling of protective responses between darinaparsin and arsenic trioxide. Although both arsenicals induced a transient heat shock response, only arsenic trioxide treatment induced transcription of metal response genes and anti-oxidant genes related to the Nrf2-Keap1 pathway. In contrast to the protective responses, both arsenicals induced up-regulation of BH3-only proteins. Moreover, silencing of BH3-only proteins Noxa, Bim, and Bmf protected myeloma cells from darinaparsin-induced cell death. Finally, treatment of an arsenic trioxide-resistant myeloma cell line with darinaparsin resulted in dose-dependent apoptosis, indicating that cross-resistance does not necessarily develop between these two forms of arsenic in multiple myeloma cell lines. These results suggest darinaparsin may be useful as an alternative treatment in arsenic trioxide-resistant hematologic cancers.[Mol Cancer Ther 2009;8(5):OF1–10]
ISSN:1535-7163
1538-8514
DOI:10.1158/1535-7163.MCT-08-1072