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Experimental treatment of neuroblastoma using (~(131)I)meta-iodobenzylguanidine and topotecan in combination

机译:(〜(131)I)间碘碘苄胍和拓扑替康联合治疗神经母细胞瘤

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摘要

The radiopharmaceutical [~(131)I]meta-iodobenzylguanidine ([~(131)I]MIBG) and the topoisomerase I inhibitor topotecan are both effective as single-agent treatments of neuroblastoma. Our purpose was to assess the therapeutic potential of [~(131)I]MIBG and topotecan in combination using SK-N-BE(2c) neuroblastoma cells and UVW/NAT glioma cells expressing the noradrenaline transporter transgene. Topotecan treatment was given (i) before, (ii) after or (iii) simultaneously with [~(131)I]MIBG. DNA fragmentation was evaluated by comet assay and cell cycle redistribution was determined by fluorescence-activated cell sorting. Combination index analysis indicated that delivery schedules (ii) and (iii) were more effective than schedule (i) with respect to clonogenic cell kill. Similarly, significant DNA damage was observed following treatment schedules (ii) and (iii) (p <0.005), but not (i). Prior exposure to topotecan did not significantly enhance [~(131)I]MIBG uptake in athymic mice bearing tumour xenografts. We conclude thai the enhancement of the efficacy of [~(131)I]MIBG by combining it with topotecan was the result of inhibition of DNA damage repair rather than an increase in expression of the noradrenaline transporter by tumour.
机译:放射性药物[〜(131)I]间碘苄基胍([〜(131)I] MIBG)和拓扑异构酶I抑制剂拓扑替康都可以作为单药治疗成神经细胞瘤。我们的目的是使用表达去甲肾上腺素转运蛋白的SK-N-BE(2c)神经母细胞瘤细胞和UVW / NAT胶质瘤细胞评估[〜(131)I] MIBG和拓扑替康的治疗潜力。在[i]之前,(ii)之后或(iii)与[〜(131)I] MIBG同时给予拓扑替康治疗。通过彗星分析评估DNA片段,并通过荧光激活的细胞分选确定细胞周期的重新分布。组合指数分析表明,就克隆细胞杀灭而言,递送时间表(ii)和(iii)比时间表(i)更有效。类似地,按照治疗方案(ii)和(iii)观察到了显着的DNA损伤(p <0.005),但没有观察到(i)。在携带肿瘤异种移植的无胸腺小鼠中,先前暴露于拓扑替康并没有显着提高[〜(131)I] MIBG的摄取。我们得出的结论是,将[〜(131)I] MIBG与托泊替康组合使用可提高其功效,这是抑制DNA损伤修复的结果,而不是肿瘤导致去甲肾上腺素转运蛋白表达增加的结果。

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