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直接作用烷化剂激活转化基因过程中的致癌物特异性

Carcinogen specificity in the activation of transforming genes by direct-acting alkylating agents.

作者信息

Garte S J, Hood A T, Hochwalt A E, D'Eustachio P, Snyder C A, Segal A, Albert R E

出版信息

Carcinogenesis. 1985 Dec;6(12):1709-12. doi: 10.1093/carcin/6.12.1709.

Abstract

DNAs from rat nasal and mouse skin carcinomas and fibrosarcomas induced by the alkylating agents methylmethane sulfonate (MMS), beta-propiolactone (BPL), and dimethylcarbamyl chloride (DMCC) were tested for their ability to transform NIH3T3 cells by DNA transfection. Each of eight MMS-induced rat nasal carcinomas and two of five BPL-induced mouse skin tumors were positive in the transfection assay while all of four fibrosarcomas and six carcinomas induced by DMCC were negative. Anchorage independent growth, tumorigenicity in nude mice, and secondary transfection confirmed the transformed phenotype of the positive transfectants. The transfectants from MMS-induced tumor DNAs did not contain restriction fragments homologous to rat H-, K- or N-ras oncogenes although exogenous (rat) tumor-derived DNA sequences were detected in transfectant genomes by Southern analysis. In contrast a BPL-induced mouse skin tumor showed evidence of containing activated H-ras. These results suggest specificity among causal chemical carcinogens for activation of transforming genes in experimental tumors.

摘要

通过DNA转染,检测了由烷化剂甲磺酸甲酯(MMS)、β-丙内酯(BPL)和二甲基氨基甲酰氯(DMCC)诱导的大鼠鼻咽癌、小鼠皮肤癌和纤维肉瘤的DNA转化NIH3T3细胞的能力。在转染试验中,8个MMS诱导的大鼠鼻咽癌中的每一个以及5个BPL诱导的小鼠皮肤肿瘤中的2个呈阳性,而DMCC诱导的所有4个纤维肉瘤和6个癌均为阴性。非贴壁依赖性生长、裸鼠致瘤性和二次转染证实了阳性转染子的转化表型。来自MMS诱导肿瘤DNA的转染子不包含与大鼠H-、K-或N-ras癌基因同源的限制性片段,尽管通过Southern分析在转染子基因组中检测到了外源(大鼠)肿瘤衍生的DNA序列。相反,一个BPL诱导的小鼠皮肤肿瘤显示出含有活化H-ras的证据。这些结果表明,在实验性肿瘤中,因果化学致癌物在激活转化基因方面具有特异性。

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