Suppression of tumorigenicity in hybrids of normal and oncogene-transformed CHEF cells.
Suppression of tumorigenicity in hybrids of normal and oncogene-transformed CHEF cells.
Somatic cell hybridization experiments were carried out to determine whether normal cells have the ability to suppress the transforming effects of a defined oncogene. A nontransformed Chinese hamster embryo fibroblast cell line (CHEF/18-dm2) was used as the normal parent, and a CHEF/18 transfectant carrying the human mutant c-Ha-ras (EJ) oncogene was used as the tumorigenic parent. Selected hybrids (L318 cell lines) were assayed for the presence of EJ DNA, for the p21 product of the c-Ha-ras gene, and for various indices of cell transformation. These hybrids exhibited a fibroblastic morphology similar to the normal parent, although they contained the EJ gene and expressed its p21 protein product at levels comparable with the transformed parent. They had a reduced capacity for anchorage-independent growth (plating efficiency in methylcellulose of less than 0.3-13%, as compared with greater than 90% for the transformed parent) and decreased tumor-forming ability in athymic mice. These findings show that normal CHEF/18 cells contain suppressor genes capable of inhibiting expression of the transformed phenotype, and tumor-forming ability, in the presence of an activated EJ oncogene.
- Harvard University United States
- Dana-Farber Cancer Institute United States
Cell Transformation, Neoplastic, Cricetulus, Suppression, Genetic, Base Sequence, Cricetinae, Animals, Oncogenes, Fibroblasts, Hybrid Cells
Cell Transformation, Neoplastic, Cricetulus, Suppression, Genetic, Base Sequence, Cricetinae, Animals, Oncogenes, Fibroblasts, Hybrid Cells
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