Literature DB >> 4069218

Specific growth response of ras-transformed embryo fibroblasts to tumour promoters.

G P Dotto, L F Parada, R A Weinberg.   

Abstract

Chemical carcinogenesis is a process involving multiple steps, as shown in several in vivo experimental systems. Two early steps have been well characterized: initiation, achieved by a single, subthreshold dose of a carcinogen, and promotion, induced by repetitive treatments with a non-carcinogenic tumour promoter. At the cellular level, establishment of the transformed phenotype is also a multi-step process and activation of several, independent genes appears to be required. Here we show that, like initiated cells, primary rat embryo fibroblasts (REFs) containing a ras but not a myc oncogene, are strongly and specifically stimulated to grow by tumour promoters. In the presence of these promoters, ras-containing REFs acquire the ability to overgrow normal cells in the monolayer and to form foci with 100% efficiency. Similar to the in vivo situation, promoter effects can be blocked by the concomitant application of retinoic acid.

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Year:  1985        PMID: 4069218     DOI: 10.1038/318472a0

Source DB:  PubMed          Journal:  Nature        ISSN: 0028-0836            Impact factor:   49.962


  55 in total

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6.  Oncogene-induced transformation of a rat embryo fibroblast cell line is enhanced by tumor promoters.

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7.  An avian retrovirus expressing chicken pp59c-myc possesses weak transforming activity distinct from v-myc that may be modulated by adjacent normal cell neighbors.

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8.  The transactivating domain of the c-Jun proto-oncoprotein is required for cotransformation of rat embryo cells.

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9.  Genetic factors and suppression of metastatic ability of v-Ha-ras-transfected rat mammary cancer cells.

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Review 10.  DNA adducts in experimental cancer research.

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