MEGESTROL-ACETATE REVERSES MULTIDRUG RESISTANCE AND INTERACTS WITH P-GLYCOPROTEIN

被引:63
|
作者
FLEMING, GF [1 ]
AMATO, JM [1 ]
AGRESTI, M [1 ]
SAFA, AR [1 ]
机构
[1] UNIV CHICAGO,MED CTR,DEPT MED,HEMATOL ONCOL SECT,5841 S MARYLAND AVE,MC2115,CHICAGO,IL 60637
关键词
MEGESTROL; MULTIDRUG RESISTANCE; P-GLYCOPROTEIN;
D O I
10.1007/BF00684845
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
We evaluated the multidrug resistance (MDR)-modulating effects of progesterone (PRG) and an orally active, structurally related compound, megestrol acetate (MA), in several MDR human cell lines. At 100-mu-M, both steroids inhibited the binding of a Vinca alkaloid photoaffinity analog to P-glycoprotein (P-gp) in MDR human neuroblastic SH-SY5Y/VCR cells [which show > 1500-fold resistance to vincristine (VCR) in the tetrazolium dye (MTT) assay]. However, 100-mu-M MA markedly enhanced the binding of [H-3]-azidopine to P-gp in both SH-SY5Y/VCR cells and the MDR human epidermoid KB-GSV2 cell line (which displays 250-fold resistance to VCR in the MTT assay). PRG had little effect on the binding of [H-3]-azidopine to P-gp. MA at low doses was more effective than PRG in sensitizing cells to VCR and enhancing their accumulation of [H-3]-VCR. The highly resistant SH-SY5Y/VCR subline exhibited significant collateral sensitivity to both steroids. These data suggest that MA may be a clinically useful modulator of MDR.
引用
收藏
页码:445 / 449
页数:5
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