Leukaemia virus infection promotes fibroblast transformation by normal BALB/c mouse DNA

Abstract

All normal cells are thought to carry genetic information for oncogenic transformation, which, on activation to continuous expression, might make the cell cancerous¹. The presently known transforming retroviruses contain transforming genes which were probably derived by recombination of a slow oncogenic retrovirus with cellular sequences closely related to these genes². It was recently reported³ that cellular DNA fragments from normal tissue culture cells could transform mouse fibroblasts in vitro with a low efficiency. High efficiency of transformation was observed in secondary transfections only when high molecular weight DNA from transformed recipient cells was used as the transforming agent³. We observed that DNA isolated from different BALB/c mouse organs can transform both NIH/3T3 and BALB/3T3 cells, although at a low frequency⁴. In attempts to increase the initial efficiency of transformation, we have found that preinfection of recipient 3T3 cells with murine leukaemia viruses markedly enhances focus formation by normal BALB/c DNA fragments.