CELLULAR PHARMACOLOGY OF 7(R)-O-METHYLNOGAROL - NEW ANTI-CANCER AGENT
- 1 January 1979
- journal article
- research article
- Vol. 210 (2) , 229-236
Abstract
The cellular accumulation and disposition of 7(R)-O-methylnogarol (7-OMEN), a derivative of the anthracycline antibiotic, nogalamycin, were compared to those of daunorubicin. Although both drugs were avidly accumulated by cells [murine L1210 leukemia cells and murine P388 leukemia cells], intracellular concentrations of 7-OMEN were 5-10 times those of daunorubicin. Lowered temperature (0.degree. C) reduced intracellular accumulation of both drugs, but 10 mM sodium azide reduced the accumulation of 7-OMEN only. Both drugs exited from cells placed in drug-free medium, a process that was reduced at 0.degree. C. Sodium azide, 10 mM, did not alter the efflux of daunorubicin from cells but hastened the efflux of 7-OMEN. Unlike whole cells, isolated nuclei accumulated more daunorubicin than 7-OMEN. This process was not reduced at 0.degree. C. Both drugs were lost from nuclei placed in drug-free buffer with only slight reduction at 0.degree. C. Unlike daunorubicin which localized in cell nuclei, 7-OMEN localized in the cytoplasm with no detectable nuclear fluorescence. Both drugs produced nearly equivalent dose-dependent inhibition of [3H]thymidine incorporation by L1210 and P388 cells. P388/ADR [adriamycin- and daunorubicin-resistant] cells proved resistant to both anthracyclines. [3H]Uridine and [3H]valine incorporations were inhibited by daunorubicin but were not altered by 7-OMEN.This publication has 5 references indexed in Scilit:
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