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对多种药物耐药的人KB细胞系的分离与遗传特征分析

Isolation and genetic characterization of human KB cell lines resistant to multiple drugs.

作者信息

Akiyama S, Fojo A, Hanover J A, Pastan I, Gottesman M M

出版信息

Somat Cell Mol Genet. 1985 Mar;11(2):117-26. doi: 10.1007/BF01534700.

Abstract

Human KB cell lines resistant to high levels of colchicine were isolated by several successive single-step selections. Most of these selection steps resulted in cross-resistance to vincristine, vinblastine, adriamycin, actinomycin D, and puromycin; however, at the highest levels of colchicine resistance, increased cross-resistance to other drugs was not observed. There was no major change in protein synthesis or alteration in protein phosphorylation or [14C]glucosamine labeling patterns accompanying the development of multiple drug resistance as measured by analysis of metabolically labeled proteins on SDS gels. Cell-cell hybridization experiments showed that the colchicine-resistant and multiple drug-resistant phenotypes were incompletely dominant. In addition, colchicine resistance was found to segregate independently from resistance to other drugs in one somatic cell hybrid, suggesting that complex genetic loci are involved in the development of the multiple drug-resistant phenotype. These mutants should be useful for the study of the clinically important problem of multiple drug resistance in human cancer.

摘要

通过连续多次单步筛选,分离出了对高浓度秋水仙碱具有抗性的人KB细胞系。这些筛选步骤大多导致对长春新碱、长春花碱、阿霉素、放线菌素D和嘌呤霉素产生交叉抗性;然而,在秋水仙碱抗性的最高水平时,未观察到对其他药物的交叉抗性增加。通过SDS凝胶上代谢标记蛋白质的分析来衡量,随着多药耐药性的发展,蛋白质合成没有重大变化,蛋白质磷酸化或[14C]葡萄糖胺标记模式也没有改变。细胞-细胞杂交实验表明,秋水仙碱抗性和多药耐药表型不完全显性。此外,在一个体细胞杂种中发现秋水仙碱抗性与对其他药物的抗性独立分离,这表明复杂的基因座参与了多药耐药表型的发展。这些突变体对于研究人类癌症中临床上重要的多药耐药问题应该是有用的。

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