Oncogenes in human primary hepatic cancer.

J R Gu, L F Hu, Y C Cheng, D F Wan
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引用次数: 0

Abstract

Transfection assay of NIH 3T3 cells was performed with DNAs isolated from ten human PHC (primary hepatic cancer) specimens and a hepatoma 7402 cell line. Positive results were obtained in 7402 and in six out of ten PHC DNAs. Human N-ras gene was identified in transfectants from 7402 DNA and transformed cells from three PHC DNA samples, which had passed more than two cycles of transfection. The expression of N-ras was also remarkably enhanced in six out of nine poly(A)+RNA samples isolated from PHC tissues. P21 synthesis was elevated in 7402 cells as well as in transfectants derived from 7402 cells and PHC DNA. In analysis of PHC DNA, rearrangement and amplification of N-ras gene was observed in two PHC samples. The discrepancy of results of the transfection assay and mRNA expression was discussed. Furthermore, c-myc was also highly expressed in most PHC tissues. It implied that the cooperating activity of N-ras and c-myc might be responsible for the malignant phenotypic alteration in some or most cases in human primary liver cancer.

人原发性肝癌的致癌基因。
用10个人原发性肝癌标本和肝癌7402细胞系分离的dna进行NIH 3T3细胞转染试验。在7402和6 / 10的PHC dna中获得了阳性结果。从7402份DNA的转染物和3份PHC DNA样本的转化细胞中鉴定出了人N-ras基因,转染周期超过2次。从PHC组织中分离的9个poly(A)+RNA样品中有6个样品的N-ras表达也显著增强。P21的合成在7402细胞以及源自7402细胞和PHC DNA的转染物中升高。在PHC DNA分析中,在两个PHC样品中观察到N-ras基因的重排和扩增。讨论了转染实验结果与mRNA表达的差异。此外,c-myc在大多数PHC组织中也高表达。提示N-ras和c-myc的协同活性可能是部分或多数人原发性肝癌恶性表型改变的原因。
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