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首页> 外文期刊>Japanese Journal of Cancer Research >Comparison of in vivo efficacy of hypoxic cytotoxin tirapazamine and hypoxic cell radiosensitizer KU-2285 in combination with single and fractionated irradiation.
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Comparison of in vivo efficacy of hypoxic cytotoxin tirapazamine and hypoxic cell radiosensitizer KU-2285 in combination with single and fractionated irradiation.

机译:低氧细胞毒素替拉帕明和低氧细胞放射增敏剂KU-2285联合单次照射和分次照射的体内疗效比较。

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摘要

Development of strategies to eradicate radioresistant hypoxic cells would be of great benefit for clinical radiotherapy. In the present study, the in vivo effects of a promising hypoxic cytotoxin, tirapazamine (3-amino-1,2,4-benzotriazine 1,4-di-N-oxide), were examined in comparison with those of KU-2285, one of the best hypoxic cell radiosensitizers, in combination with both single and fractionated irradiation. The tumor response was assessed by the standard in vivo-in vitro clonogenic assay using SCCVII tumors in C3H mice and EMT-6/KU tumors in Balb/c mice with different characteristics of tumor hypoxia. With single-dose irradiation (18 Gy), both tirapazamine and KU-2285 showed significant enhancement of cell killing in a dose-dependent manner, but tirapazamine was more effective for SCCVII tumors with acutely hypoxic cells, while KU-2285 was more effective for EMT-6/KU tumors predominantly with chronically hypoxic cells. In fractionated irradiation regimens (4 fractions of 5 Gy at 12 h intervals), tirapazamine showed more marked combined effects at 10 and 20 mg/kg than KU2285 at 100-200 mg/kg in both SCCVII and EMT-6/KU tumors. We concluded that the effectiveness of KU-2285 and tirapazamine was correlated with the nature of tumor hypoxia with single-dose irradiation, whereas tirapazamine appeared more potent than KU-2285 with fractionated irradiation. These findings suggest the potential usefulness of tirapazamine in clinical fractionated radiotherapy.
机译:根除放射线耐性低氧细胞的策略的开发将对临床放射治疗大有裨益。在本研究中,与KU-2285相比,研究了一种有前途的低氧细胞毒素替拉帕明(3-氨基-1,2,4-苯并三嗪1,4-二-N-氧化物)的体内作用,最好的缺氧细胞放射增敏剂之一,与单次照射和分级照射结合使用。通过标准的体内-体外克隆形成试验,使用具有不同肿瘤缺氧特征的C3H小鼠中的SCCVII肿瘤和Balb / c小鼠中的EMT-6 / KU肿瘤,评估肿瘤反应。单剂量照射(18 Gy)时,替拉帕明和KU-2285均以剂量依赖性方式显着增强细胞杀伤力,但替拉帕明对具有急性低氧细胞的SCCVII肿瘤更有效,而KU-2285则更有效。 EMT-6 / KU肿瘤主要带有慢性低氧细胞。在分级照射方案中(每12小时间隔4个5 Gy组分),在100和200 mg / kg的SCCVII和EMT-6 / KU肿瘤中,替拉帕明在10和20 mg / kg的情况下显示出比KU2285更明显的联合作用。我们得出的结论是,单剂量照射时KU-2285和替拉帕明的有效性与肿瘤缺氧的性质有关,而分剂量照射时,替拉帕明似乎比KU-2285更有效。这些发现表明替拉帕明在临床分级放疗中的潜在用途。

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