Regulatory mechanism of simian virus 40 gene expression in permissive and in nonpermissive cells

Author:

Graessmann A,Graessmann M,Mueller C

Abstract

Primary or continuous lines of mouse cells (3T3) are nonpermissive for simian virus 40 (SV40). Abortively infected cells synthesize tumor antigen (T antigen but not viral DNA and virus capsid protein (V antigen). V antigen, however, was obtained when SV40 DNA was injected into 3T3 cells. This late gene expression also appears to be correlated with the quantity of injected DNA molecules per 3T3 cell. T antigen formation can be detected after microinjection of only 1 to 2 DNA molecules, but the intensity of intranuclear T antigen fluorescence is significantly brighter with injection of higher concentrations of viral DNA. In permissive cells (TC7), early and late SV40 gene expression is directly related to the number of injected molecules. Microinjection of 1DNA molecule induced T and V antigen formation with the same efficiency as microinjection of 2,000 to 4,000 molecules. The question of weather late SV40 gene expression is directly related to the quantity of an early virus-specific product was approached by microinjection of early SV40 complementary RNA together with small amounts of viral DNA. V antigen was obtained in a high proportion of recipient 3T3 cells at conditions where microinjection of viral DNA alone induced T but not V antigen synthesis.

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

Reference16 articles.

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4. Ueber die Bildung von Melanin in Muskelzellen nach der direkten Uebertragung von RNA aus Harding-Passey-Melanomzellen;Graessmann A.;Hoppe-Seyler's Z. Physiol. Chem.,1971

5. Inhibition by interferon of SV 40 tumor antigen formation in cells injected with SV 40 cRNA transcribed in vitro;Graessmann A.;FEBS Lett.,1974

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