哺乳动物体外细胞的表型耐药。

P C Verschure, J W Simons
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引用次数: 4

摘要

当哺乳动物细胞在低浓度的有毒药物中培养时,它们通常会产生表型抗性。我们研究了这种表型抗性是否是由于对先前存在的变异的选择。以8-阿扎瓜因(AG)和6-硫鸟嘌呤(TG)作为耐药参数,测定次黄嘌呤掺入量。在次黄嘌呤的摄取中发现了克隆间预先存在的变异,这种变异具有遗传成分。这种次黄嘌呤异常掺入的传递并没有表现出稳定的性状,变异细胞系逐渐恢复到原来的稳定状态。有迹象表明,在细胞群中,次黄嘌呤掺入水平改变的细胞不断出现,而且频率很高。用微量毒性浓度的AG或TG治疗表明,至少对于AG,生存与先前存在的次黄嘌呤摄取变化无关。观察到的现象可能对癌症化疗药物的选择具有重要意义。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Phenotypic drug resistance in mammalian cells in vitro.

When mammalian cells are cultured at low concentrations of toxic drugs, they often become phenotypically resistant. We studied whether this phenotypic resistance is due to selection of preexisting variants. The drugs 8-azaguaine (AG) and 6-thioguanine (TG) were used and, as a parameter for resistance, the incorporation of hypoxanthine was determined. Preexisting variation among clones in the uptake of hypoxanthine was found, and this variation has a hereditary component. This transmission of aberrant incorporation of hypoxanthine does not appear a stable trait, and the aberrant cell lines returned gradually to the original steady state. There are indications that within a cell population cells with altered levels of incorporation of hypoxanthine arise continuously and at a high frequency. Treatment with marginally toxic concentrations of AG or TG indicates that, at least for AG, survival is not related to the preexisting variation in hypoxanthine uptake. The observed phenomena could be of importance for the selection of drugs to be used in cancer chemotherapy.

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