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• W2104892016 abstract "ara-Cytidine-5 9 -alkylphosphonophosphates and the corresponding -diphosphates were found to be cytostatically active in vitro against the human mammary epithelial cell line H184 A1N4 and the human mammary tumor cell line MaTu. Our results indicate that the replacement of the diphosphate by the phosphonophosphate group has no influence on anti- proliferative activity in this case. The compounds were more active than the corresponding cytidine phospholipid conju- gates and related compounds lacking a cytostatically active nucleoside, the ara-C prodrug Cytoros, and were slightly less active than ara-C. The cytostatic effect was prevented by 2 9 - deoxycytidine indicating their action as prodrugs of ara-C. In contrast to ara-C, they increase (Ca 2 1 ) 1 in H184 A1N4 cells, pointing to a different mechanism of action in addition to their prodrug effect. In combination with phospholipid ana- logs, synergistic effects could be observed. Further studies within the disease-oriented in vitro Anticancer Screening Pro- gram of the National Cancer Institute show selectivity for cer- tain cancer cell lines. The hexadecyl derivatives revealed a sig- nificant antitumor activity in vivo against the murine lymphatic leukemia P 388 cells being equally potent or even superior to ara-C. In contrast to ara-C, they were found to be orally active. Side effects measured as leukopenia and body weight reduction were less pronounced than with the parent drug. —Brachwitz, H., J. Bergmann, I. Fichtner, Y. Thomas, C. Vollgraf, P. Langen, and W. E. Berdel. 1- b - D -Arabinofuranosyl- cytosine-5 9 -alkylphosphonophosphates and diphosphates: new orally active derivatives of ara-C. J. Lipid Res. 1998. 39: 162-172." @default.
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• W2104892016 title "1-β-d-Arabinofuranosylcytosine-5′-alkylphosphonophosphates and diphosphates: new orally active derivatives of ara-C" @default.
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• W2104892016 doi "https://doi.org/10.1016/s0022-2275(20)34212-7" @default.
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