Brain Infection by Neuroinvasive but Avirulent Murine Oncornaviruses
- 1 January 2000
- journal article
- research article
- Published by American Society for Microbiology in Journal of Virology
- Vol. 74 (1) , 465-473
- https://doi.org/10.1128/jvi.74.1.465-473.2000
Abstract
The chimeric murine oncornavirus FrCas E causes a rapidly progressive noninflammatory spongiform encephalomyelopathy after neonatal inoculation. The virus was constructed by the introduction of pol-env sequences from the wild mouse virus CasBrE into the genome of a neuroinvasive but nonneurovirulent strain of Friend murine leukemia virus (FMuLV), FB29. Although the brain infection by FrCas E as well as that by other neurovirulent murine retroviruses has been described in detail, little attention has been paid to the neuroinvasive but nonneurovirulent viruses. The purpose of the present study was to compare brain infection by FrCas E with that by FB29 and another nonneurovirulent virus, F43, which contains pol-env sequences from FMuLV 57. Both FB29 and F43 infected the same spectrum of cell types in the brain as that infected by FrCas E , including endothelial cells, microglia, and populations of neurons which divide postnatally. Viral burdens achieved by the two nonneurovirulent viruses in the brain were actually higher than that of FrCas E . The widespread infection of microglia by the two nonneurovirulent viruses is notable because it is infection of these cells by FrCas E which is thought to be a critical determinant of its neuropathogenicity. These results indicate that although the sequence of the envelope gene determines neurovirulence, this effect appears to operate through a mechanism which does not influence either viral tropism or viral burden in the brain. Although all three viruses exhibited similar tropism for granule neurons in the cerebellar cortex, there was a striking difference in the distribution of envelope proteins in those cells in vivo. The FrCas E envelope protein accumulated in terminal axons, whereas those of FB29 and F43 remained predominantly in the cell bodies. These observations suggest that differences in the intracellular sorting of these proteins may exist and that these differences appear to correlate with neurovirulence.Keywords
This publication has 28 references indexed in Scilit:
- Mapping of a Neurovirulence Determinant within the Envelope Protein of a Polytropic Murine Retrovirus: Induction of Central Nervous System Disease by Low Levels of VirusVirology, 1998
- Dissecting the Determinants of Neuropathogenesis of the Murine OncornavirusesVirology, 1998
- Gene Expression in ScrapieJournal of Biological Chemistry, 1998
- Different biosynthetic transport routes to the plasma membrane in BHK and CHO cells.The Journal of cell biology, 1996
- Mechamisms of cell polarity: sorting and transport in epithelial cellsCurrent Opinion in Cell Biology, 1994
- Murine retrovirus-induced spongiform encephalopathy: Productive infection of microglia and cerebellar neurons in accelerated CNS diseaseNeuron, 1991
- Cell-surface receptor for ecotropic murine retroviruses is a basic amino-acid transporterNature, 1991
- Polarized sorting of viral glycoproteins to the axon and dendrites of hippocampal neurons in cultureCell, 1990
- Moloney Murine Leukemia Virus Temperature-Sensitive Mutants: A Model for Retrovirus-Induced Neurologic DisordersPublished by Springer Nature ,1990
- Characterization of monoclonal antibodies reactive with murine leukemia viruses: Use in analysis of strains of friend MCF and friend ecotropic murine leukemia virusVirology, 1983