Author: Lavi, Ehud; Das Sarma, Jayasri; Weiss, Susan R.
Title: Cellular Reservoirs for Coronavirus Infection of the Brain in β(2)-Microglobulin Knockout Mice Cord-id: grarghun Document date: 1999_2_22
ID: grarghun
Snippet: Mouse hepatitis virus (MHV) A59 infection which causes acute encephalitis, hepatitis, and chronic demyelination, is one of the experimental models for multiple sclerosis. Previous studies showed that lethal infection of β(2)-microglobulin ‘knockout’ (β(2)M(-/-)) mice required 500-fold less virus and viral clearance was delayed as compared to infection of immunocompetent C57Bl/6 (B6) mice. To investigate the mechanism of the increased susceptibility of β(2)M(-/-) mice to MHV-A59, we studie
Document: Mouse hepatitis virus (MHV) A59 infection which causes acute encephalitis, hepatitis, and chronic demyelination, is one of the experimental models for multiple sclerosis. Previous studies showed that lethal infection of β(2)-microglobulin ‘knockout’ (β(2)M(-/-)) mice required 500-fold less virus and viral clearance was delayed as compared to infection of immunocompetent C57Bl/6 (B6) mice. To investigate the mechanism of the increased susceptibility of β(2)M(-/-) mice to MHV-A59, we studied organ pathology and the distribution of viral antigen and RNA during acute and chronic infection. A59-infected β(2)M(-/-) mice were more susceptible to acute encephalitis and hepatitis, but did not have increased susceptibility to demyelination. Viral antigen and RNA distribution in the brain was increased in microglia, lymphocytes, and small vessel endothelial cells while the distribution in neurons and glia was similar in β(2)M(-/-) mice and B6 mice. Acute hepatitis and thymus cortical hypoplasia in β(2)M(-/-) mice were delayed in onset but pathologic changes in these organs were similar to those in B6 mice. The low rate of demyelination in β(2)M(-/-) mice was consistent with the low dose of the virus given. A less neurotropic virus MHV-2, caused increased parenchymal inflammation in β(2)M(-/-) mice, but without demyelination. Thus, CD8+ cells were important for viral clearance from endothelial cells, microglia and inflammatory cells, but not from neuronal and glial cells. In addition, CD8+ cells played a role in preventing the spread of encephalitis.
Search related documents:
Co phrase search for related documents- abundant cytoplasm and acute infection: 1, 2
- active viral replication and acute disease: 1, 2, 3
- active viral replication and acute hepatitis: 1
- active viral replication and acute infection: 1, 2, 3, 4, 5, 6, 7, 8, 9
- active viral replication evidence and acute infection: 1
- acute disease and additional mouse: 1
- acute disease and additional reservoir: 1
- acute infection and additional mouse: 1
- acute infection and additional organ: 1
- acute infection and additional reservoir: 1
Co phrase search for related documents, hyperlinks ordered by date