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J. Virol., Dec 1995, 8089-8095, Vol 69, No. 12
GW Anderson and PG Plagemann
In C58 and AKR mice, endogenous N-tropic, ecotropic murine leukemia virus
(MuLV) proviruses become activated in rare cells during embryogenesis.
Resultant replication-competent progeny viruses then actively infect a
large number of cells throughout the fetus, including cells in the
developing central nervous system. By in situ hybridization analyses, we
have assessed the presence of ecotropic MuLV RNA in the brains of C58 mice
as a function of age. Only a few ecotropic MuLV-positive cells were
observed in weanling mice, but the number of positive cells in the brain
increased progressively with increasing age of the mice. Throughout the
lives of the mice, the ecotropic MuLV RNA-positive cells were primarily
located in well- defined white-matter tracts of the brain (commissura
anterior, corpus callosum, fimbria hippocampi, optical tract, and striatum)
and of the spinal cord. Cells of the subventricular zone also expressed
ecotropic MuLV RNA, and in older mice a small number of positive cells were
present in the grey matter. Infection of endogenous ecotropic MuLV
provirus-less CE/J mice in utero with ecotropic MuLV clone AKR-623 resulted
in the extensive infection of brain cells. The regional distribution of
ecotropic MuLV RNA-containing cells was the same as observed in the brains
of C58 mice, in which cells became infected by endogenously activated
virus, but the number of positive cells was higher.
Copyright © 1995, American Society for Microbiology
Expression of ecotropic murine leukemia virus in the brains of C58/M, DBA2/J, and in utero-infected CE/J mice
Department of Microbiology, University of Minnesota, Minneapolis 55455, USA.
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