Abstrakt: |
ABSTRACTThe chimeric murine oncornavirus FrCasEcauses a rapidly progressive paralytic disease associated with spongiform neurodegeneration throughout the neuroaxis. Neurovirulence is determined by the sequence of the viral envelope gene and by the capacity of the virus to infect microglia. The neurocytopathic effect of this virus appears to be indirect, since the cells which degenerate are not infected. In the present study we have examined the possible role of inflammatory responses in this disease and have used as a control the virus F43. F43 is an highly neuroinvasive but avirulent virus which differs from FrCasEonly in 3'poland envsequences. Like FrCasE, F43 infects large numbers of microglial cells, but it does not induce spongiform neurodegeneration. RNAase protection assays were used to detect differential expression of genes encoding a variety of cytokines, chemokines, and inflammatory cell-specific markers. Tumor necrosis factor alpha (TNF-a) and TNF-ß mRNAs were upregulated in advanced stages of disease but not early, even in regions with prominent spongiosis. Surprisingly there was no evidence for upregulation of the cytokines interleukin-1a (IL-1a), IL-1ß, and IL-6 or of the microglial marker F4/80 at any stage of this disease. In contrast, increased levels of the ß-chemokines MIP-1a and -ß were seen early in the disease and were concentrated in regions of the brain rich in spongiosis, and the magnitude of responses was similar to that observed in the brains of mice injected with the glutamatergic neurotoxin ibotenic acid. MIP-1a and MIP-1ß mRNAs were also upregulated in F43-inoculated mice, but the responses were three- to fivefold lower and occurred later in the course of infection than was observed in FrCasE-inoculated mice. These results suggest that the robust increase in expression of MIP-1a and MIP-1ß in the brain represents a correlate of neurovirulence in this disease, whereas the TNF responses are likely secondary events. |