Affiliation:
1. Department of Microbiology, Michigan State University, East Lansing 48824-1101.
Abstract
Viral replication in mice infected with murine polyomavirus strains with novel enhancer rearrangements was analyzed by direct in situ hybridization of whole mouse sections and by hybridization of nucleic acids extracted from a specific set of organs. The enhancer rearrangements included a deletion of the B domain as well as duplications within the A domain. Comparisons between enhancer variants demonstrate that the B domain plays an important role in replication in most organs, in particular in the kidney, at the neonatal stage (days 0 to 7 postbirth). In contrast, the B domain is not required in those organs which can sustain replication in the adult, i.e. mammary gland, skin, and bone (class I organs [J. J. Wirth, A. Amalfitano, R. Gross, M. B. A. Oldstone, and M. M. Fluck, J. Virol. 66:3278-3286, 1992]). Altogether, the results suggest that the B and A domains mediate very different functions in infection of mice, controlling the acute and persistent phases of infection, respectively. A model of mouse infection based on the crucial role of differentially expressed host transcription factors is presented.
Publisher
American Society for Microbiology
Subject
Cell Biology,Molecular Biology
Reference50 articles.
1. Polyoma regulatory region: a potential probe for mouse cell differentiation;Amati P.;Cell,1985
2. Host range mutants of polyoma virus;Benjamin T. L.;Proc. Natl. Acad. Sci. USA,1970
3. Specific tissue targeting of polyoma virus oncogenicity in athymic nude mice;Berebbi M.;Oncogene,1988
4. Interaction of distinct nuclear proteins with sequences controlling the expression of polyomavirus early genes;Bohnlein E.;Mol. Cell. Biol.,1986
5. Interaction of nuclear factor EF-1A with the polyomavirus enhancer region;Bolwig G. M.;J. Virol.,1991
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