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X射线转化的哺乳动物细胞中的独特转化基因。

Distinctive transforming genes in x-ray-transformed mammalian cells.

作者信息

Borek C, Ong A, Mason H

出版信息

Proc Natl Acad Sci U S A. 1987 Feb;84(3):794-8. doi: 10.1073/pnas.84.3.794.

Abstract

DNAs from hamster embryo cells and mouse C3H/10T1/2 cells transformed in vitro by x-irradiation into malignant cells transmit the radiation transformation phenotype by producing transformed colonies (transfectants) in two mouse recipient lines, the NIH 3T3 and C3H/101/2 cells, and in a rat cell line, the Rat-2 cells. DNAs from unirradiated cells or irradiated and visibly untransformed cells do not produce transformed colonies. The transfectants grow in agar and form tumors in nude mice. Treatment of the DNAs with restriction endonucleases prior to transfection indicates that the same transforming gene (oncogene) is present in each of the transformed mouse cells and is the same in each of the transformed hamster cells. Southern blot analysis of 3T3 or Rat-2 transfectants carrying oncogenes from radiation-transformed C3H/10T1/2 or hamster cells indicates that the oncogenes responsible for the transformation of 3T3 cells are not the Ki-ras, Ha-ras, or N-ras genes, nor are they neu, trk, raf, abl, or fms, although quick blot analysis using 11 oncogene probes detected increased transcripts of c-abl and c-fms in the 3T3 transformants containing oncogenic sequences from the x-ray-transformed C3H/10T1/2 cells. The work demonstrates that DNAs from mammalian cells transformed into malignancy by direct exposure in vitro to radiation contain genetic sequences with detectable transforming activity in three recipient cell lines. The results provide evidence that DNA is the target of radiation carcinogenesis induced at a cellular level in vitro. The experiments indicate that malignant radiogenic transformation in vitro of hamster embryo and mouse C3H/10T1/2 cells involves the activation of unique non-ras transforming genes, which heretofore have not been described.

摘要

仓鼠胚胎细胞和经X射线体外转化为恶性细胞的小鼠C3H/10T1/2细胞的DNA,通过在两种小鼠受体细胞系(NIH 3T3和C3H/101/2细胞)以及一种大鼠细胞系(Rat-2细胞)中产生转化菌落(转染子),传递辐射转化表型。未受辐射细胞或受辐射但明显未转化细胞的DNA不会产生转化菌落。转染子能在琼脂中生长并在裸鼠体内形成肿瘤。转染前用限制性内切酶处理DNA表明,每个转化的小鼠细胞中都存在相同的转化基因(癌基因),且每个转化的仓鼠细胞中的癌基因也相同。对携带来自辐射转化的C3H/10T1/2细胞或仓鼠细胞癌基因的3T3或Rat-2转染子进行Southern印迹分析表明,负责3T3细胞转化的癌基因不是Ki-ras、Ha-ras或N-ras基因,也不是neu、trk、raf、abl或fms基因,尽管使用11种癌基因探针进行的快速印迹分析在含有来自X射线转化的C3H/10T1/2细胞致癌序列的3T3转化子中检测到c-abl和c-fms的转录本增加。这项工作表明,通过体外直接暴露于辐射而转化为恶性的哺乳动物细胞的DNA,在三种受体细胞系中含有具有可检测转化活性的基因序列。结果提供了证据,证明DNA是体外细胞水平诱导的辐射致癌作用的靶点。实验表明,仓鼠胚胎和小鼠C3H/10T1/2细胞的体外恶性辐射转化涉及独特的非ras转化基因的激活,此前尚未对此进行描述。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/aafd/304302/05c12c380f80/pnas00268-0187-a.jpg

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