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Time-lapse live cell imaging and flow analysis of multidrug resistance reversal by verapamil in bladder cancer cell lines.

机译:定期活细胞成像和维拉帕米逆转膀胱癌细胞系中多药耐药性的流分析。

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OBJECTIVES: To examine the effects of verapamil on the intracellular drug pharmacokinetics of epirubicin using alternative dosing schedules. The results might inform the choices for optimizing clinical chemotherapy. METHODS: Sensitive parental (MGH-U1) and multidrug resistant (MDR) (MGH-U1R and MGH-U1-MMC) bladder cancer cell lines were used. Fluorescence time-lapsed studies were performed on cells incubated with epirubicin alone or combined with verapamil. Flow cytometry was performed after the alternative dosing regimens. RESULTS: Verapamil reversed the epirubicin localization patterns in MDR cells. Time-lapse imaging showed that nuclear epirubicin accumulation in MDR cells with verapamil followed the parental curve. The maximal reversal took >60 minutes. Flow cytometry showed increased epirubicin uptake in MDR cells co-incubated with verapamil. Preincubation was not as effective as co-incubation. CONCLUSIONS: The results of our model indicate that longer exposure to MDR-class drugs, exemplified by epirubicin, increases uptake and the MDR reversing action of co-treatment with verapamil. The present results highlight the need for additional clinical trials of drug dosing and scheduling for combination intravesical chemotherapy regimens.
机译:目的:使用替代给药方案检查维拉帕米对表柔比星细胞内药物药代动力学的影响。结果可能会为优化临床化疗提供选择。方法:使用敏感的亲代(MGH-U1)和多药耐药(MDR)(MGH-U1R和MGH-U1-MMC)膀胱癌细胞系。对仅与表柔比星一起孵育或与维拉帕米联合孵育的细胞进行了荧光延时研究。在替代给药方案后进行流式细胞术。结果:维拉帕米逆转了MDR细胞中表柔比星的定位模式。延时成像显示维拉帕米MDR细胞中核表柔比星的积累遵循亲本曲线。最大反转耗时> 60分钟。流式细胞仪显示与维拉帕米共孵育的MDR细胞中表柔比星的吸收增加。预孵育不如共同孵育有效。结论:我们的模型结果表明,与表柔比星一起长期暴露于MDR类药物可增加与维拉帕米共同治疗的摄取和MDR逆转作用。目前的结果凸显了对于联合膀胱内化疗方案的药物剂量和时间表的其他临床试验的需要。

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