首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >5-Bromo-2′-deoxyuridine Potentiation of Transformation of Rat-Embryo Cells Induced In Vitro by 3-Methylcholanthrene: Induction of Rat Leukemia Virus gs Antigen in Transformed Cells
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5-Bromo-2′-deoxyuridine Potentiation of Transformation of Rat-Embryo Cells Induced In Vitro by 3-Methylcholanthrene: Induction of Rat Leukemia Virus gs Antigen in Transformed Cells

机译:5-溴-2-脱氧尿苷对3-甲基胆碱体外诱导的大鼠胚胎细胞转化的增强作用:在转化细胞中诱导大鼠白血病病毒gs抗原

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摘要

Low-passage rat-embryo cells were not transformed by 3-methylcholanthrene or by 5-bromo-2′ deoxyuridine. However, prior treatment with bromodeoxyuridine, followed by treatment with methylcholanthrene, resulted in cell transformation about three subpassages after removal of the carcinogen. RNA-directed DNA polymerase activity could not be detected in either normal or transformed cells. However, gs-1 antigen specific for rat C-type RNA virus was detected in cultures derived from bromodeoxyuridine-treated cells. No gs-1 antigen for the C-type RNA virus was detected in cultures that had not been treated with bromodeoxyuridine during the 25 subpassages of these experiments.High-passage rat-embryo cells, derived from a different cell pool, were transformed by either methylcholanthrene or dimethylbenzanthracene without prior infection with an exogenous virus, and without prior treatment with bromodeoxyuridine, gs-1 antigen for C-type RNA virus was also detected in 4 of 4 randomly selected transformed cell lines; the gs-1 antigen was not detected in any of 4 nontransformed control cultures. Considering these and previously published findings, we conclude that the lowpassage cells cannot be transformed by methylcholanthrene because of powerful cellular controls over the endogenous virus. Bromodeoxyuridine triggers some expressions of the endogenous virus; thus, the bromodeoxyuridine-treated cells are more susceptible to the transforming effects of methylcholanthrene. High-passage rat cells do not maintain perfect control over expression of their endogenous virus; the cell cultures are susceptible to the transforming effects of chemical carcinogens.
机译:低代大鼠胚细胞没有被3-甲基胆甾或5-溴-2'脱氧尿苷转化。但是,先用溴脱氧尿嘧啶核苷处理,再用甲基胆甾醇处理,在除去致癌物后约三个亚代会导致细胞转化。在正常或转化细胞中均未检测到RNA定向的DNA聚合酶活性。但是,在衍生自溴脱氧尿苷处理的细胞的培养物中检测到了对大鼠C型RNA病毒具有特异性的gs-1抗原。在这些实验的25次传代过程中,未使用溴脱氧尿苷处理的培养物中未检测到C型RNA病毒的gs-1抗原。通过另一种方法转化源自不同细胞库的高传代大鼠胚胎细胞在未事先感染外源病毒且未事先使用溴脱氧尿嘧啶核苷处理的情况下,也可以在4种随机选择的转化细胞系中的4种中检测到Cs RNA的gs-1抗原。在4种未转化的对照培养物中均未检测到gs-1抗原。考虑到这些以及以前发表的发现,我们得出结论,由于对内源性病毒的强大细胞控制,低代细胞不能被甲基胆甾醇转化。溴脱氧尿苷可触发内源性病毒的某些表达。因此,溴脱氧尿嘧啶核苷处理的细胞更容易受到甲基胆固醇的转化作用的影响。高传代的大鼠细胞不能完全控制其内源性病毒的表达。细胞培养物易受化学致癌物转化的影响。

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