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ras基因扩增与恶性转化。

ras gene Amplification and malignant transformation.

作者信息

Pulciani S, Santos E, Long L K, Sorrentino V, Barbacid M

出版信息

Mol Cell Biol. 1985 Oct;5(10):2836-41. doi: 10.1128/mcb.5.10.2836-2841.1985.

Abstract

Morphologic transformation of NIH 3T3 mouse cells occurs upon transfection of these cells with large amounts (greater than or equal to 10 micrograms) of recombinant DNA molecules carrying the normal human H-ras-1 proto-oncogene. We provide experimental evidence indicating that transformation of these NIH 3T3 cells results from the combined effect of multiple copies of the H-ras-1 proto-oncogene rather than from spontaneous mutation of one of the transfected H-ras-1 clones (E. Santos, E.P. Reddy, S. Pulciani, R.J. Feldman, and M. Barbacid, Proc. Natl. Acad. Sci. USA 80:4679-4683, 1983). Levels of H-ras-1 RNA and p21 expression are highly elevated in the NIH 3T3 transformants, and in those cases examined, these levels correlate with the malignant properties of these cells. We have also investigated the presence of amplified ras genes in a variety of human carcinomas. In 75 tumor biopsies, we found amplification of the human K-ras-2 locus in one carcinoma of the lung. These results indicate that ras gene amplification is an alternative pathway by which ras genes may participate in the development of human neoplasia.

摘要

用携带正常人H-ras-1原癌基因的大量(大于或等于10微克)重组DNA分子转染NIH 3T3小鼠细胞后,这些细胞会发生形态学转变。我们提供的实验证据表明,这些NIH 3T3细胞的转化是由多个拷贝的H-ras-1原癌基因的联合作用导致的,而不是由转染的H-ras-1克隆之一的自发突变引起的(E. 桑托斯、E.P. 雷迪、S. 普尔恰尼、R.J. 费尔德曼和M. 巴尔巴西德,《美国国家科学院院刊》80:4679 - 4683,1983)。在NIH 3T3转化细胞中,H-ras-1 RNA和p21表达水平高度升高,在所检测的这些情况中,这些水平与这些细胞的恶性特性相关。我们还研究了多种人类癌组织中ras基因的扩增情况。在75份肿瘤活检样本中,我们在一例肺癌中发现了人类K-ras-2基因座的扩增。这些结果表明,ras基因扩增是ras基因可能参与人类肿瘤发生发展的另一条途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/13a1/367023/da0bb85aca40/molcellb00106-0351-a.jpg

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