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人胚胎癌中c-Ki-ras2原癌基因的扩增及表达增强

Amplification and enhanced expression of the c-Ki-ras2 protooncogene in human embryonal carcinomas.

作者信息

Wang L C, Vass W, Gao C L, Chang K S

出版信息

Cancer Res. 1987 Aug 1;47(15):4192-8.

PMID:2886216
Abstract

Two cell lines of human embryonal carcinoma, Tera-1 and Tera-2, have been found to exhibit a 4- to 6-fold amplification of protooncogene c-Ki-ras2. The polyadenylic acid selected RNA also showed 8-fold or greater enhancement, showing marked elevation in the level of two major mRNAs, 5.7 and 4.0 kilobases, and two additional minor mRNAs, 2.3 and 1.2 kilobases, as compared with those of a normal human embryonic fibroblast cell line, MRC-5. More than one-half of the number of tumor samples obtained from metastatic human embryonal carcinomas also showed c-Ki-ras2 gene amplification and enhanced mRNA expression. However, the c-Ki-ras2 gene amplification did not always lead to enhanced mRNA expression, and some embryonal carcinomas showed mRNA overexpression without apparent c-Ki-ras2 gene amplification. These results suggest that human embryonal carcinomas may have c-Ki-ras2 amplification and/or overexpression before in vitro culture. Among various chromosomal changes observed in Tera-1 and Tera-2 cells, there were anomalies in chromosome 12 in which c-Ki-ras2 is located although these karyological changes alone could not account for the amplification observed. It is suggested that the genomic instability and active DNA replication during the early developmental period may give rise to changes involving c-Ki-ras2 which may contribute to oncogenic processes.

摘要

已发现两种人胚胎癌细胞系Tera - 1和Tera - 2的原癌基因c - Ki - ras2呈现4至6倍的扩增。与正常人胚胎成纤维细胞系MRC - 5相比,经聚腺苷酸筛选的RNA也显示出8倍或更高的增强,表明5.7和4.0千碱基的两种主要mRNA以及2.3和1.2千碱基的另外两种次要mRNA的水平显著升高。从转移性人胚胎癌获得的肿瘤样本中,超过一半也显示出c - Ki - ras2基因扩增和mRNA表达增强。然而,c - Ki - ras2基因扩增并不总是导致mRNA表达增强,一些胚胎癌显示出mRNA过表达但无明显的c - Ki - ras2基因扩增。这些结果表明,人胚胎癌在体外培养之前可能就已经存在c - Ki - ras2扩增和/或过表达。在Tera - 1和Tera - 2细胞中观察到的各种染色体变化中,尽管单独这些核型变化无法解释所观察到的扩增,但位于12号染色体上的c - Ki - ras2存在异常。提示在发育早期的基因组不稳定性和活跃的DNA复制可能导致涉及c - Ki - ras2的变化,这可能有助于致癌过程。

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