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米索硝唑和环磷酰胺对C3H小鼠乳腺癌体内有氧及缺氧细胞的细胞毒性作用

Cytotoxic effect of misonidazole and cyclophosphamide on aerobic and hypoxic cells in a C3H mammary carcinoma in vivo.

作者信息

Grau C, Bentzen S M, Overgaard J

机构信息

Danish Cancer Society, Department of Experimental Clinical Oncology, Aarhus.

出版信息

Br J Cancer. 1990 Jan;61(1):61-4. doi: 10.1038/bjc.1990.13.

Abstract

The chemosensitising effect of the nitroaromatic radiosensitiser misonidazole (MISO) on the alkylating agent cyclophosphamide (CTX) has been investigated in a C3H mammary carcinoma in CDF1 mice. The selective cytotoxicity against aerobic and hypoxic cells was measured indirectly, using a local tumour control (TCD50) assay. The hypoxic fraction was calculated from the dose difference between the TCD50S for tumours irradiated either in air or under clamped conditions. The relative survival of tumour cells after drug therapy was expressed as a surviving fraction (SF). CTX (100 mg kg-1) was found to be considerably more toxic towards hypoxic than aerobic cells (SF 4% versus 52%). MISO (1000 mg kg-1) was almost exclusively toxic to hypoxic cells (SF 22%). When MISO and CTX were administered simultaneously a decrease in the surviving fraction was observed. The effect on aerated cells was found to be 10-fold more than expected from addition of toxicities, suggesting a chemosensitising effect on these cells by MISO when used in combination with CTX. No synergistic effect was found on radiobiologically hypoxic cells. The exact role of hypoxia for the development of chemosensitisation seems to be complex and requires additional research in the future.

摘要

在CDF1小鼠的C3H乳腺癌模型中,研究了硝基芳香族放射增敏剂米索硝唑(MISO)对烷化剂环磷酰胺(CTX)的化学增敏作用。使用局部肿瘤控制(TCD50)试验间接测量对需氧细胞和缺氧细胞的选择性细胞毒性。缺氧分数根据在空气中或夹闭条件下照射的肿瘤的TCD50之间的剂量差异计算得出。药物治疗后肿瘤细胞的相对存活率表示为存活分数(SF)。发现CTX(100 mg kg-1)对缺氧细胞的毒性比对需氧细胞大得多(SF分别为4%和52%)。MISO(1000 mg kg-1)几乎只对缺氧细胞有毒性(SF为22%)。当同时给予MISO和CTX时,观察到存活分数降低。发现对通气细胞的影响比毒性相加预期的大10倍,这表明MISO与CTX联合使用时对这些细胞有化学增敏作用。在放射生物学缺氧细胞上未发现协同作用。缺氧在化学增敏作用发展中的确切作用似乎很复杂,未来需要更多研究。

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Potentiation in vivo of melphalan activity by nitroimidazole compounds.硝基咪唑化合物对美法仑体内活性的增效作用。
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