BCNU is a caspase-mediated inhibitor of drug-induced apoptosis

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作者
Peták, I
Mihalik, R
Bauer, PI
Süli-Vargha, H
Sebestyén, A
Kopper, L
机构
[1] Semmelweis Univ Med, Inst Pathol & Expt Canc Res 1, H-1085 Budapest, Hungary
[2] Semmelweis Univ Med, Dept Biochem Med, H-1085 Budapest, Hungary
[3] Hungarian Acad Sci, Res Grp Peptide Chem, H-1117 Budapest, Hungary
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中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
BCNU [1,3-bis(2-chloroethyl)-1-nitrosourea], a bifunctional (alkylating/carbamoylating) anticancer agent, in noncytotoxic doses (12-50 mu M) inhibited drug-induced apoptosis in HT58 human lymphoma cells exposed to etoposide (ETO; 50 mu M) as well as in mouse thymocytes exposed to dexamethasone (5 mu g/ml) in vitro in 4-h cultures, The cytoplasmic extracts of ETO-treated HT58 cells cleaved both purified poly(ADP-ribose)polymerase and Ac-Asp-Glu-Val-Asp-7-amino-4-methylcoumarin fluorogenic caspase substrate, indicating the presence of active caspases, and these effects were inhibited by BCNU concentration dependently, The carbamoylating decomposite, 2-chloroethyl-isocyanate (6-25 mu M), also decreased ETO-induced apoptosis in HT58 cells in vitro and their caspase 3-like activity ex vivo, whereas N-(2-chloroethyl)-N-nitrosocarbamoyl-valinamide, an alkylating and mainly intramolecularly carbamoylating nitrosourea derivative (400 mu M), did not influence these phenomena. Furthermore, the activity of recombinant caspase 3 was also strongly inhibited by BCNU and 2-chloroethyl-isocyanate. These results indicate that BCNU, via its carbamoylating capacity, can inactivate cysteine protease(s) essential for ETO-induced apoptosis, This apoptosis-modulating property of BCNU, in turn, may influence the efficacy of chemotherapeutic protocols in the treatment of cancer.
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页码:614 / 618
页数:5
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