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人类肿瘤细胞存活曲线的初始斜率:其被需氧细胞增敏剂β-阿拉伯呋喃糖腺嘌呤所改变。

The initial slope of human tumor cell survival curves: its modification by the oxic cell sensitizer beta-arabinofuranosyladenine.

作者信息

Chavaudra N, Halimi M, Parmentier C, Gaillard N, Grinfeld S, Malaise E P

机构信息

Institut Gustave-Roussy, Villejuif, France.

出版信息

Int J Radiat Oncol Biol Phys. 1989 May;16(5):1267-71. doi: 10.1016/0360-3016(89)90296-4.

Abstract

The initial slope of the survival curve, which is a characteristic of each tumor cell line, varies with the histological group of the tumor. It is one of the factors on which clinical radioresponsiveness depends. The DNA dependant DNA polymerase inhibitor beta-ara A acts as an oxic cell sensitizer. This study was carried out on human tumor cell lines to look for a correlation between the degree of radiosensitization induced by beta-ara A and the radiosensitivity of a given cell line. Six human tumor cell lines with different radiosensitivities were used (the survival rate at 2 Gy and D ranged from 20 to 73% and from 1.2 to 3.2 Gy, respectively). beta-ara A had a major toxic effect on all cell lines but this varied greatly from one cell line to another and was concentration dependant; this toxic effect was taken into account when calculating the surviving fractions. For all cell lines, beta-ara A acted as an oxic radiosensitizer and the radiosensitization was concentration dependant. Analysis of the survival curves of the 6 cell lines using the linear quadratic model showed that concentrations of beta-ara A between 200 and 1000 microM induced an increase in the linear component while the quadratic component underwent no systematic change. The sensitizing enhancement ratio (SER) measured from the Ds ratios, varied greatly from one line to another. For example, at a concentration of 500 microM, the extreme values of Ds ratios were 1.5 and 2.6. The radiosensitization is greater, the higher the radiosensitivity of the cell line studied during exponential growth. The results do not favor the use of beta-ara A in the treatment of intrinsically radioresistant human tumors.

摘要

生存曲线的初始斜率是每个肿瘤细胞系的一个特征,它随肿瘤的组织学类型而变化。它是临床放射反应性所依赖的因素之一。DNA依赖性DNA聚合酶抑制剂β-阿糖腺苷(β-ara A)作为一种需氧细胞增敏剂。本研究在人肿瘤细胞系上进行,以寻找β-ara A诱导的放射增敏程度与给定细胞系的放射敏感性之间的相关性。使用了六种不同放射敏感性的人肿瘤细胞系(2 Gy时的存活率和D值分别在20%至73%和1.2至3.2 Gy范围内)。β-ara A对所有细胞系都有主要的毒性作用,但这种作用在不同细胞系之间差异很大,且呈浓度依赖性;在计算存活分数时考虑了这种毒性作用。对于所有细胞系,β-ara A作为需氧放射增敏剂,且放射增敏呈浓度依赖性。使用线性二次模型分析这6种细胞系的生存曲线表明,200至1000 microM之间的β-ara A浓度会导致线性成分增加,而二次成分没有系统性变化。从Ds比值测量的增敏增强比(SER)在不同细胞系之间差异很大。例如,在500 microM的浓度下,Ds比值的极值为1.5和2.6。在指数生长期间所研究的细胞系放射敏感性越高,放射增敏作用越大。结果不支持将β-ara A用于治疗内在放射抗拒的人类肿瘤。

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