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. 1994 Apr-Jun;8(2-3):121-7.
doi: 10.1007/BF02780662.

129/Ola mice carrying a null mutation in PrP that abolishes mRNA production are developmentally normal

J C Manson  1 A R ClarkeM L HooperL AitchisonI McConnellJ Hope
Affiliations

129/Ola mice carrying a null mutation in PrP that abolishes mRNA production are developmentally normal

J C Manson et al. Mol Neurobiol. 1994 Apr-Jun.

Abstract

The neural membrane glycoprotein PrP is implicated in the pathogenesis of the transmissible spongiform encephalopathies; however, the normal function of PrP and its precise role in disease are not understood. Recently, gene targeting has been used to produce mice with neo/PrP fusion transcripts, but no detectable PrP protein in the brain (1). Here we report the use of a different targeting strategy, to produce inbred mice with a complete absence of both PrP protein and mRNA sequences. At 7 mo of age, these mice show no overt phenotypic abnormalities despite the normal high levels of expression of PrP during mouse development. The mice are being used in experiments designed to address the role of PrP in the pathogenesis of scrapie and the replication of infectivity.

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References

    1. EMBO J. 1990 Feb;9(2):395-9 - PubMed
    1. Nature. 1992 Apr 16;356(6370):577-82 - PubMed
    1. Lancet. 1991 Feb 16;337(8738):425 - PubMed
    1. Roux Arch Dev Biol. 1989 May;198(1):48-56 - PubMed
    1. J Gen Virol. 1987 Oct;68 ( Pt 10):2711-6 - PubMed

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