Nitrobenzo[a]pyrene-induced DNA amplification in SV40-transformed chinese hamster embryo cells

## Abstract Infection with Herpes simplex viruses (HSV) induces amplification of SV40 sequences in SV40‐transformed Chinese hamster embryo cells (CO631). This is shown by __in situ__ hybridization of the infected cells with cloned ^32^P‐labelled SV40 DNA. The HSV‐mediated synthesis of SV40 DNA is m

## Abstract The environmental pollutants 1,6‐dinitropyrene (1,6‐DNP) and 1,8‐dinitropyrene (1,8‐DNP) are strongly carcinogenic in a number of animal models. These DNPs are metabolized by nitroreduction to __N__‐hydroxy arylamine derivatives that either directly or after acetylation bind to cellular

## Abstract Amplification of SV40 genes in SV40‐transformed Chinese hamster embryo cells (CO631) by chemical carcinogens as well as by herpes simplex virus infection can be inhibited by infection with the defective parvovirus, AAV‐5. This is shown by __in situ__ hybridization with SV40 DNA of AAV‐5

## Abstract Eleven simian virus 40‐transformed cell lines from 5 different species were tested for their ability to amplify integrated simian virus 40 DNA upon infection with herpes simplex virus type I or treatment with various chemical carcinogens. Four cell lines were positive only for virus‐ind

## Bisphenol-A (BP -A) is a major component of epoxy, polycarbonate and other resins. For an assessment of in vitro carcinogenicity and related activity of BP-A, the abilities of this compound to induce cellular transformation and genetic effects were examined simultaneously using the Syrian hamst

DNA adduct induction by N-acetoxy-N-2-acetylaminofluorene (N-Ac-AAF) has been investigated in Chinese hamster ovary (CHO) cells using immunoelectron microscopy. The major RNA and DNA adducts, N-(guanosin-8-yl)-2-aminofluorene (G-C8-AF) and N-(deoxyguanosin-8-yI)-2-aminofluorene (dG-C8-AF), were loca