Structural Determinants of Phenoxazine Type Compounds Required to Modulate the Accumulation of Vinblastine and Vincristine in Multidrug-Resistant Cell Lines
- 1 January 1990
- journal article
- research article
- Published by Cognizant, LLC in Cancer Communications
- Vol. 2 (7) , 249-259
- https://doi.org/10.3727/095535490820874308
Abstract
Phenoxazine and seven other structurally related compounds were investigated to determine whether they would increase accumulation of Vinca alkaloids in multidrug-resistant (MDR) GC3/C1 (human colon adenocarcinoma) and KB-ChR-8-5 (HeLa variant) cell lines. Among eight compounds examined, phenoxazine caused greater accumulations of vincristine (VCR) and vinblastine (VLB) than the other chemosensitizers. The structure-activity relationship of these compounds for anti-MDR activity suggested an ideal tricyclic ring structure with a basic nitrogen atom at position 10 for modulating the accumulation of Vinca alkaloids. Addition of oxygen to position 5 of the tricyclic ring system further increased the activity, implying that a highly electronegative element with one, or more, lone pair of electrons in the nucleus opposite to heterocyclic nitrogen was a requirement for better anti-MDR activity. The relationship between the concentration of phenoxazine and the potentiation of Vinca alkaloid accumulation in comparison to verapamil was examined. For VCR in GC3/C1 cells, maximal modulation indices were: for verapamil, 1.8; phenoxazine, 8.6; and for VLB, 1.3 for verapamil compared to 3.3 for phenoxazine. In KB-ChR-8-5 cells, for VCR the maximal modulating index values were 9.0 and 4.3, respectively, and for phenoxazine and verapamil and for VLB were 5.0 and 3.7, respectively. Accumulations of VLB in GC3/C1 cells were similar in the presence of 1 μM phenoxazine or 10 mM sodium azide plus 10 mM 2-deoxyglucose. The effects of verapamil and phenoxazine on the accumulation of Vinca alkaloid were additive. Further, phenoxazine decreased the efflux of VLB by 30% in KB-ChR-8-5 cell line and 10% in GC3/C1 cells. In addition to enhancing the cytotoxicities of VCR and VLB, phenoxazine competed relatively weakly for binding to P-glycoprotein with [3H]azidopine and moderately with [3H]azidoverapamil, at equal concentrations, suggesting that the multidrug transporter may be the primary target for phenoxazine.This publication has 26 references indexed in Scilit:
- Preparing nuclei from cells in monolayer cultures suitable for counting and for following synchronized cells through the cell cycleAnalytical Biochemistry, 1984
- INCREASED ACCUMULATION OF VINCRISTINE AND ADRIAMYCIN IN DRUG-RESISTANT P388-TUMOR CELLS FOLLOWING INCUBATION WITH CALCIUM-ANTAGONISTS AND CALMODULIN INHIBITORS1982
- Enhanced efflux of actinomycin D, vincristine, and vinblastine in adriamycin-resistant subline of P388 leukemiaCancer Letters, 1979
- ALTERED SURFACE-MEMBRANE GLYCOPROTEINS IN VINCA ALKALOID-RESISTANT HUMAN-LEUKEMIC LYMPHOBLASTS1979
- ACTIVE EFFLUX OF DAUNORUBICIN AND ADRIAMYCIN IN SENSITIVE AND RESISTANT SUBLINES OF P388-LEUKEMIA1979
- MECHANISMS OF RESISTANCE TO DAUNORUBICIN IN EHRLICH ASCITES TUMOR-CELLS1978
- MECHANISM OF CROSS-RESISTANCE BETWEEN VINCRISTINE AND DAUNORUBICIN IN EHRLICH ASCITES TUMOR-CELLS1978
- Correlation of biologic data with physico-chemical properties among the Vinca alkaloids and their congenersBiochemical Pharmacology, 1977
- Modulation of drug permeability in chinese hamster ovary cells. Possible role for phosphorylation of surface glycoproteinsBiochimica et Biophysica Acta (BBA) - Biomembranes, 1977
- CHARACTERIZATION OF A GLUCOCORTICOID-SENSITIVE HUMAN LYMPHOID-CELL LINE1977