Transformation of type 1 astrocytes with N‐ethyl‐N‐nitrosourea: Establishment of an in vitro system and the role of the p53 gene

1995 
N-ethyl-N-nitrosourea (ENU)-induced gliomas, animal models of human gliomas, are most frequently oligodendrocytic, while human gliomas tend to be astrocytic. To facilitate a detailed study of human glial carcinogenesis, we developed an in vitro system using type 1 astrocyte transformation with ENU. Type 1 astrocytes from fetal Wistar rat brain were treated by a single dose of ENU. Transformed colonies appeared 50 days after exposure to single doses of ENU greater than 150 μg/mL. Cloned cells from these colonies retained the immunohistochemical characteristics of type 1 astrocytes. They showed rapid growth and high saturation densities, colony formation in low (2%) serum medium and gave rise to tumors when injected into nude mice. When p53 expression was studied at each passage, a single cell positive for mutant p53 protein emerged 40 days after ENU treatment. In the next 1–3 passages, the mutant p53 positive cell formed piled-up colonies and exhibited dominant growth. Northern blot analysis showed markedly increased accumulations of p53 mRNA in transformed cells. This in vitro transformation system of type 1 astrocytes provides a valuable tool for further investigations of astrocyte carcinogenesis. © 1995 Wiley-Liss, Inc.
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