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秋水仙碱抗性在艾氏腹水瘤和细胞系中的持续性。

Persistence of colchicine resistance in Ehrlich-Lettré ascites tumors and cell strains.

作者信息

Granzow C

出版信息

J Cancer Res Clin Oncol. 1981;102(1):57-69. doi: 10.1007/BF00410535.

Abstract

The effect of colchicine on mitoses of mutant HD33 Ehrlich-Lettŕe ascites cells growing in vivo and in vitro was studied. HD33 mouse ascites tumors are colchicine-resistant. The LD50 of colchicine in mice bearing HD33 ascites tumors was 1.4 mg/kg body weight (b.w.), but a single dose of 3.33 mg colchicine/kg b.w. failed to suppress the anaphase of HD33 tumor mitoses for 24 h. No change in the level of colchicine resistance was observed after 269 weekly transplantations of HD33 ascites tumors without colchicine. In suspension culture, growth of HD33 ascites cells ceased at 1.5 x 10(-6) M colchicine. 10(-5) M colchicine suppressed the anaphase of HD33 mitoses and produced typical C-mitoses within one hour. The same effects on mitoses of colchicine sensitive Ehrlich ascites cells in vitro were achieved with 10(-6) M colchicine. In HD33 ascites cell cultures grown without colchicine, only a slight increase in colchicine sensitivity was registered after 5 years. Parallel cultures were propagated for the same period in the presence of 10(-7) M colchicine (HD33C ascites cells) without detectable growth alterations; the resistance level increased slightly. The limit of 10(-6) M colchicine was tolerated by the ascites cells in permanent culture without growth reduction (HD33CS ascites cells). 3H-colchicine binding studies suggest a permeability barrier of the plasma membrane as a mechanism of genetically fixed resistance.

摘要

研究了秋水仙碱对体内和体外生长的突变型HD33 Ehrlich-Lettre腹水细胞有丝分裂的影响。HD33小鼠腹水肿瘤对秋水仙碱耐药。携带HD33腹水肿瘤的小鼠中,秋水仙碱的半数致死量为1.4mg/kg体重,但单次剂量3.33mg秋水仙碱/kg体重未能在24小时内抑制HD33肿瘤有丝分裂的后期。在不使用秋水仙碱的情况下对HD33腹水肿瘤进行269次每周传代后,未观察到秋水仙碱耐药水平的变化。在悬浮培养中,HD33腹水细胞在1.5×10⁻⁶M秋水仙碱时停止生长。10⁻⁵M秋水仙碱在一小时内抑制了HD33有丝分裂的后期并产生了典型的C-有丝分裂。在体外,10⁻⁶M秋水仙碱对秋水仙碱敏感的艾氏腹水细胞的有丝分裂也有相同的作用。在不使用秋水仙碱培养的HD33腹水细胞培养物中,5年后仅记录到秋水仙碱敏感性略有增加。在10⁻⁷M秋水仙碱存在的情况下(HD33C腹水细胞)平行培养相同时间,未检测到生长改变;耐药水平略有增加。在永久培养中,腹水细胞能够耐受10⁻⁶M秋水仙碱的极限浓度而不降低生长速度(HD33CS腹水细胞)。³H-秋水仙碱结合研究表明,质膜的通透性屏障是遗传固定耐药性的一种机制。

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本文引用的文献

2
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Proc Natl Acad Sci U S A. 1966 Dec;56(6):1735-42. doi: 10.1073/pnas.56.6.1735.
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Science. 1959 Jul 3;130(3366):40-1. doi: 10.1126/science.130.3366.40.
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Sublines of the Ehrlich-Lettré mouse ascites tumour. A new tool for experimental cell research.
Naturwissenschaften. 1972 Feb;59(2):59-63. doi: 10.1007/BF00593464.

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