Spontaneous, mutagen-induced and adenovirus-induced anchorage independent tumorigenic variants of mouse cells

Abstract

Normal C57 Black mouse embryo cells did not form colonies in agarose, but rare variant (ar⁺) cells able to grow in agarose were detected. Fluctuation analysis showed that ar⁺ variants arose by spontaneous mutation in the cultured cells. The frequency of ar⁺ variants was increased by treating cells with N‐methyl‐N'nitro‐N‐nitrosoguanidine or ethyl methane sulphonate, or by abortive infection by human adenovirus type 5. Induced ar⁺ cells were fibroblastic; most grew slowly and had slightly reduced saturation density and increased serum requirement, but formed colonies in agarose. Fourteen of twenty ar⁺ clones induced by Ad5 were T antigen negative and two of these were also negative when tested for viral DNA. Six clones contained a few cells that were T antigen positive when first tested, but were negative when retested later. The ar⁺ variants were tumorigenic in athymic and in normal syngeneic mice. The results suggest that the ar⁺ phenotype can arise by spontaneous or chemically‐induced mutation, and can be induced by adenovirus by a process different from classical transformation.